Is Schizophrenia a circadian disease that I expect to have a higher incidence & prevalence in a 4G-5G blue-lit world?  Yes, that is my belief.  Blue light/nnEMF alters the periodicity of clocks in the brain. The periodicity of our clocks determines the shape of our lives. Time sculpts life, not energy. What happens in your colony of mitochondria every AM writes a story in your eyes and eventually your frontal lobes where this disease begins.

People forget schizophrenia tends to happen in young men and this is because their brains do not myelinate as fast as women do until 28 years old.  This makes them more susceptible to charge changes in their eyes and frontal lobes as the picture above shows.  Young people tend to get schizophrenia due to clock disruption while older people who have such bad clock disruption that it leads to apoptosis of neurons in the damaged area of the brain get frontotemporal displasia.  I believe these diseases are linked via the amount of trauma and destruction to the brain over time.

Frontotemporal dementia, especially the behavioral variant (bvFTD), is difficult to recognize in its early stages because it is often confused with schizophrenia. Thus, the similarities are obvious: in sufferers of both groups, personality as well as behavioral changes occur.

The SCN optical clock is activated by the sun and the absence of light at night. Meck was the first to postulate that the rate at which signals traverse this loop offers the brain a timekeeping mechanism to control the chronobiology of hormones, protein turnover, neurotransmitter release, and metabolism pathways. Before Meck’s work on timing, no one thought to link these functions to the SCN.  This implies that even minor brain injuries could lead to SCN dysfunction.  The SCN operates as an optical lattice clock who’s proteins gears and their associated chemical bonds seem to pulse and resonate (periodicity) with electromagnetic frequencies.  The pulse rate and resonance are key features of how the clock handles time sensation and circadian control of timing in cells connected to it.  The clock was built by evolution to operate with terrestrial sunlight frequencies but it also appears to be affected by other parts of the electromagnetic spectrum when they are present.  Trauma also affects its physiologic abilities. It appears the SCN is the distal target for information processing of light between the retina and basal ganglia and neocortex of man.  This makes it very critical in mental illness and diseases associated with altered light environments.  It also means it is very critical in pituitary dysfunction and hormone release.  Dopamine controls pituitary hormone release with prolactin.

Melatonin and dopamine control all the photoreceptors in humans that allow for proper communication. Melatonin controls mitochondrial DNA change programs and dopamine controls how we decipher and sense time between the inside and the outside world we inhabit.  Creating melatonin & dopamine in the eye is the most critical physical change at a surface for humans because of how it controls our sense of time via photoreceptor regeneration.  Melatonin controls all regeneration of the photoreceptors in man except the Muller cells in the eye.  Both of these chemical molecules are made by sunlight as it collides with aromatic amino acids in our eye to slow light down.  That is how they link to one another.

There was ample opportunity for DNA modification in life for the first 2.5 billion years of life on Earth. Yet, there is no evidence of significant change in life forms during that time span in the fossil record. It was not until about 600 million years ago when the oxygen tension rose to a point where air-breathing life forms became thermodynamically possible and favored, that a significant change can be abruptly seen in the fossil record. In other words, DHA creation and use in the central retinal pathways were critical to allowing our DNA to change.  Today, the light flowing through our eyes has changed and now diseases like schizophrenia can manifest.

The SCN optical clock activated by the sun and the absence of light at night. Meck was the first to postulate that the rate at which signals traverse this loop offers the brain a timekeeping mechanism to control chronobiology of hormones, protein turnover, neurotransmitter release, and metabolism pathways. Before Meck, no one thought to link these functions to the SCN.  This implies that even minor brain injuries could lead to SCN dysfunction.  The SCN operates as an optical lattice clock who’s proteins gears and their associated chemical bonds seem to pulse and resonate with electromagnetic frequencies.  This is called periodicity. 

Clocks become more accurate the more periodicity they have. Mitochondria regulate circadian rhythmicity through NAD+ production, SIRT1 & SIRT3 activation & mitochondrial dynamics. Those things make molecular clocks more accurate. SIRT1 and SIRT3 activity in HDACs is dependent on NAD+ recycling in cells.  NAD+ recycling is highly dependent on tryptophan being used accurately as a time crystal at cytochrome 1. SIRT1 and SIRT3 counteract CLOCK (gene product); NAD+ synthesis is highly dependent on proper circadian rhythmicity set by the light and dark cycles of the sun.

The pulse rate and resonance are key features of how the clock handles time sensation and circadian control of timing in cells connected to it.  The clock was built by evolution to operate with terrestrial sunlight frequencies but it also appears to be affected by other parts of the electromagnetic spectrum when they are present.

DHA’s main effect on cells was done by evolution to improve a cell’s ability to tell time.   How? DHA improved the periodicity of the SCN. This is why today in humans the central retinal pathways have more DHA in their cell membranes than any neurologic tract in our species. The periodicity of our clocks determines the phenotype in our brain circuits. In this way, time sculpts life, not energy. What happens in our colony of mitochondria every AM writes a story in our circuitry that goes awry in schizophrenia.

Trauma also affects our physiologic abilities because it lowers the periodicity of clocks. It appears the SCN is the distal target for information processing of light between the retina and basal ganglia and neocortex of man.  This makes it very critical in mental illness and diseases associated with altered light environments.  It also means it is very critical in pituitary dysfunction and hormone release from any cause.

We know now that increased dopamine increases the rate of the basal ganglia loop cycling. This forges connections between disparate parts of the brain to create a larger web of interconnections.  Melatonin and cortisol are critical in trimming those connections at night to optimize function. This suggests that the more dopamine we make, the faster our internal clock would seem to run to us.  People with schizophrenia tend to have more dopamine released rapidly over short time scales.  This leads to the disease phenotype.

As a result, our perceptions would be associated with a slower perception of external time. This is what the “time dilation experience” of childhood appears to be.

This occurs with increases in body temperature and yokes perfectly to UV light’s ability to make dopamine in the eye/skin during the daytime. Darkness lowers levels of dopamine levels and a slower rate of neural circuit frequency would correspond to a slower internal clock and a perceived acceleration of external time. This is likely why low dopamine states” are associated with time contraction and disease states and are linked to circadian de-coupling events.  One must also realize that dopamine levels also control pituitary hormone release.  This is why hormone abnormalities are often found in trauma victims and mental illness patients.

Today the 4G-5G RF/microwaved blue-lit world is the major de-coupler of human physiology of the SCN.  The association of dopamine and melatonin function is a non-linear relationship because both molecules are created and linked to specific light frequencies diurnally that vary and this makes the relationship not so clear-cut for those who do not understand the non-linear aspects of photonics or optics well.

The under- or over-activity of the dopamine system is linked with impairment inaccurate time estimation, sometimes making it seem slower, sometimes faster. There is no obvious or linear correlation between perceived speed of time and the amount of dopamine present as one might suspect, but I believe there is a fractal relationship of dopamine levels to protein dynamics due to a lack of UV and IR light perception in the retina, because of Meck’s work.   Why do I say this?

Schizophrenics have an altered sense of time that begins in the SCN but is amplified in the midbrain dopamine regulation centers of the basal ganglia and reward processing tracts of the orbital frontal gyri which are known to be disrupted in schizophrenia.  They also have altered fragmented thoughts because of this inability to time reality properly.  This is one reason why nnEMF affects attention and awareness because light can alter charge variation in aromatic amino acids and this ACUTELY can raise and lower dopamine/melatonin levels seemingly altering reality as it unfolds.  We see this in TBI victims as well.  Unfortunately, that is the world a schizophrenic observes 24/7 when their illness takes hold.   Focus and attention come easier when one’s CNS is not being pulled down multiple pathways by contravening evoked potentials from man-made electromagnetic waves. This is why we often too EEG/ERP on our TBI victims.

Paying attention, establishes traction between your internal frequencies and the external world, synchronizing with it, and using it to help calibrate your internal pace of timing.

Deficits in time perception in Schizophrenic patients is helpful for the quantum clinician in understanding how sunlight builds time management in the brain.

Deficits in time perception have been observed in a range of disorders, and there is typically a trend to misjudge durations in most of them because of the uncoupling of the circadian mechanism:

•Manic patients tend to overestimate the duration

•Depressive patients tend to underestimate the duration

However, schizophrenic patients show poor estimation without a trend. Results are not systematic (Vogeley and Kupke, 2007)

Schizophrenic patients were asked to answer two kinds of discrimination questions:

•Do two stimuli have the same duration?

•Are they short or long?

They performed worse than controls but without a systematic bias toward over or underestimating. (Elvevag, 2003)

Dopamine transmission plays a massive role in schizophrenia. Goldsmith et al (1997) found an increased number of dopamine receptors in post-mortem and PET scan studies of schizophrenics.

Interestingly, an increase in dopaminergic transmission increases the speed of one’s ‘internal clock’, whilst inhibition slows it down. (Rammsayer, 1993)

As schizophrenia is characterized by a disruption of dopamine and melatonin communication in the brain, the unsystematic nature of impairment is not surprising. It demonstrates that in healthy individuals, integration across the brain is key for temporal perception.  We can use cortisol assays in Schizophrenia the same way we can use them in TBI victims when we treat them using light hygiene protocols.

Do not think that the use of exogenous melatonin is free of risk.  It is the biggest mistake modern centralized medicine makes today.


More and more evidence indicates that the circadian clock and mitochondrial functioning are related. Most available evidence shows how the circadian clock controls the abundance and morphology of mitochondria by regulating biogenesis, fission/fusion and mitophagy. Additionally, several studies suggest that mitochondrial functioning also is regulated by the circadian clock as Knock Out gene/protein studies show altered mitochondrial respiration and ROS metabolism, although in these studies, it is difficult to separate effects on substrate availability and mitochondrial function itself. Conversely, direct evidence for mitochondrial regulation of feedback to the circadian clockwork remains limited in centralized research done by Big Pharma dollars.  I think this being done by design to keep the focus on drug development instead of solar phototherapy.

For a better understanding of how mitochondrial morphology and functioning change throughout the day, more experiments on diurnal animals are needed in sunlight.  Performing imaging and respiration assays throughout the day in different tissues seems to be essential in order to get a clearer picture whether morphology and respiration oscillate throughout the day, whether this is tissue dependent and whether this is related to the molecular clock, substrate availability or a combination of both. Furthermore, data on other regulators such as hormone signaling and the autonomic nervous system, both outputs of the central clock, are scarce, and need to be done. Light frequencies humans use now clearly exert influences on mitochondrial functioning. One first candidate hormone to investigate is melatonin & dopamine since both control photoreceptor regeneration that is linked to SCN function.  Tryptophan and tyrosine biology are key gears in clock mediated disease.

Highlights of the latest research on this topic:

Dietary tryptophan and threonine can control circadian behavioral rhythms.

Tryptophan is metabolized in a time- and light- dependent manner.

Light cycles and tryptophan intake coordinate temporal regulation of metabolism and transcription.

Tryptophan metabolism regulate expression of the core clock machinery.






Did you know albumin is also a ‘dynamic’ fluorophore protein in the blood?  Its ability to absorb UV light changes with temperature and pH.  After Vermont 2018 talk this should stop you dead in your tracks.  What might it mean?   Research has shown albumin has 4.66 percent TYROSINE and 0.19 percent tryptophan at a pH of 2.

Lerner and Barnum noted in 1946 that a shift in the maximum absorption of serum albumin to longer wavelengths when the pH was changed from 2 to 10 in the blood plasma.  As the temperature rises, molecular vibrations increase which results in the ability of water to ionize and form more hydrogen ions (H+). As a result, the pH will drop.

  • The local environment (pH/temperature)of the aromatic amino acids can have an effect on their spectra. This means that tryptophan will have an emission peak at lower wavelengths when buried within the hydrophobic inner regions of a protein while tyrosine will often transfer its energy to adjacent tryptophan amino acids. Ionized tyrosinate, which forms when protons are lost from tyrosine as a result of increasing pH, will demonstrate wavelengths similar to tryptophan.

Phenylalanine and tyrosine are the simplest aromatic amino acids derived from alanine. Phenylalanine is an essential amino acid that our body cannot synthesize. This does not apply to tyrosine, which the body can synthesize only if there is a sufficient amount of phenylalanine.  Tyrosine has one of the highest absorption spectra for UV light in biochemistry.  Interesting huh?

The maximum and minimum absorption of tyrosine moves progressively to longer wavelengths in the ultraviolet range as the pH is increased above pH 7.0. This is why inflammation in the body lowers your ability to harvest UV light.  It is also why people with high HS CRP often have low Vitamin D levels even when they live in a good solar environment and you have tan skin.

In solutions of pH 12.0, a second sharp absorption maximum appears at 240 nm, which is ascribed to the ionization of the phenolic group of tyrosine. The ultraviolet spectra of tryptophan shift only slightly with pH, while those of phenylalanine are relatively independent of pH.  Tyrosine physiology is most sensitive to inflammation in the body.

pH decreases with an increase in temperature. You do know that UV light increases temperature the most on our surfaces huh?  But this does not mean that water becomes more acidic at higher temperatures. A solution is considered acidic if there is an excess of hydrogen ions over hydroxide ions.

Does anyone want to guess what is made from tyrosine?

Thyroid hormones. Melanin, dopamine, adrenaline, and noradrenalin. Inflammation in your body lowers the production of all these chemicals.

Aside from being a proteinogenic amino acid, tyrosine has a special role by virtue of phenol functionality. It occurs in proteins that are part of signal transduction processes. It functions as a receiver of phosphate groups that are transferred by way of protein kinases. Phosphorylation of the hydroxyl group can change the activity of the target protein or may form part of a signaling cascade via SH2 domain binding.  This is a topologic change mediated via charge alterations that are very important.  If you’ve carefully read the last few blogs this information should stir you.


A tyrosine residue also plays an important role in photosynthesis. In chloroplasts (photosystem II), it acts as an electron donor in the reduction of oxidized chlorophyll. In this process, it loses the hydrogen atom (H+) of its phenolic OH-group. This radical is subsequently reduced in the photosystem II by the four core manganese clusters.  Plants and the microbiome make tyrosine from the shikimate pathway and mammals usually get it from the conversion of phenylalanine from foods.  That is another aromatic amino acid.  When this conversion is made in humans it creates more water.  That water is also special.  When tyrosine is changed into all the catecholamines in our cells did you know it throws off water in the conversion? What might the purpose of this be to Nature?

The thyroid hormones triiodothyronine (T3) and thyroxine (T4) in the colloid of the thyroid also are derived from tyrosine in the anterior pituitary.

Tyrosine is also the precursor to the pigment MELANIN found in the RPE of your eye and the pigment of your skin.

Tyrosine (or its precursor phenylalanine) is needed to synthesize the benzoquinone structure which forms part of coenzyme Q10 that shuttles electrons from cytochrome 1 to cytochrome 3.  This is part of the Q cycle I did an entire webinar on.   Do you know that UVA and UVB products tend to inhibit ECT at this level too huh?

Tyrosine hydroxylase catalyzes the initial and rate-limiting step in the biosynthetic pathway of catecholamines including dopamine, noradrenaline, and adrenaline. Regulation of thyroid hormone activity is important for a variety of physiological and behavioral functions of these catecholamines.

The ultraviolet absorption spectrum of serum albumin was built to be dynamic to the solar spectrum for some reason.  Not only that but it can be interpreted almost quantitatively on the basis solely of the tyrosine present in the protein.

Tyrosine makes some important things in our blood plasma, doesn’t it?  Things that should make you go hum after my Vermont 2018 talk………..is this why dopamine can be made in the powerful sun and during CT when the sun is weak?  The answer is Yep.  It can be made in two ways so that mammals can dominate in all seasons.

Is this why studies have found tyrosine to be useful during conditions of stress, cold, fatigue, prolonged work, and sleep deprivation, with reductions in stress hormone levels?  Yep.  When you know better about the light you always do better than any food guru can teach you.


Hydrogen bonding networks are very dynamic relative to the electromagnetic and charge environment they find themselves in. They are so dynamic that we cannot perceive how fast they adapt. It happens at femtoseconds. The fast adaptive behavior of these H+ networks in water, alone determines the dielectric constant of the medium they are within. Seasonal weather variations due to the sun drive these processes for biology because how light alters the charges of things inside of cells.  Normal bulk water has a high dielectric value. Low pH aqueous environments (inflammation) contain more protons or fewer electrons and as a result, have a lowered dielectric value.

Alkaline pH also changes the dielectric constant in biological systems because of how charges evolve. The coherent domains or EZ water in cells has a dielectric constant of 160.  The non coherent domains in water vary from 14 to 78.  Charge conservation does not act like energy conservation ideas found in the laws of thermodynamics. Energy cannot be created or destroyed. Neither can charges.

Here is the key difference:  Charge confirmation does not mean that individual positive and negative charges cannot be created or destroyed. Why? Electric charge is ONLY carried by subatomic particles such as electrons and protons, and those particles move in biological systems changing the dielectric potential of tissues as the charges move. Charging of water by sunlight creates a massive net negative charge in water’s coherent domains also called the exclusion zone (EZ). Charged particles that carry electrical & magnetic information can be created and destroyed in elementary particle reactions. CERN does this every day. So does the sun.  Biology has yet to realize the implications of this in cells.  People forget that light can change or alter the charge on biomolecules.


Trying to define charge is like trying to define love – you can only really describe the effect it has on other things. And both charge and love rest heavily on the “opposites attract” rule.

In the atoms and molecules that make up all matter, there are only two players when it comes to charge: protons with a positive charge, and electrons with a negative charge. Their charges are opposite, so they attract. And their charges are equal (both have a charge of 1), so when they get together they balance out each other’s charge, giving atoms an overall neutral (zero) charge.

There’s a yang to all that attraction yin — positive charges repel other positives, and likewise for negative charges.

That’s the accounting side of the charge story – now for the fun stuff: separating opposite charges to create electric fields.

The attraction between opposite charges means that they’re usually found stuck together, and pulling them apart always takes energy.  Mitochondria separate electrons from protons in foods via electron chain transportation nanomachines.

Once they’re apart that energy gets stored in an electric field around each of the individual charges. The field instantly spreads out from the charge in all directions at the speed of light, and literally goes on forever.

But fields get weak with distance so the charge’s attractive/repulsive effect dies off pretty quickly. It’s the electric field of energy around them that lets isolated charges attract and repel each other without ever touching!

But batteries aren’t the only things that can keep charges separated, and make use of the electric field in between them. Capacitors are like a kind of temporary battery – they keep positive and negative charges separated by an insulator, with an electric field between and around them.  Mitochondria should be thought of as a diurnal  capacitor that tells time.

The more negative and positive charges you separate, the stronger the electric field that forms between and around them, and the more electrical energy that can be tapped. That separation of charge is what creates voltage, or potential difference.

Batteries get their voltage by having positive and negative charges separated – their positive and negative electrodes are separated by an insulating layer. Each time you use a battery, a bit more of the separated charge gets reunited via the circuit, and the electric field between the positive and negative electrodes gets a bit weaker. Rechargeable batteries pump the charges back to their separate sides during charging, strengthening the electric field all over again.  Cells strengthen their electric fields when they are exposed to sunlight daily. The battery in cells are water based (EZ).

But batteries aren’t the only things that can keep charges separated, and make use of the electric field in between them. Capacitors are like a kind of temporary battery – they keep positive and negative charges separated by an insulator, with an electric field between and around them.  Mitochondria should be thought of as a diurnal capacitor that tells time.

Touchscreens in phones and tablets act like capacitors when they use electric fields to detect your fingers. And it’s not just electronics that rely on capacitance – every living cell acts like a capacitor too.

Most electrical charge is found in water networks inside of cells. This is called the exclusion zone (EZ) in cells.  This charge in the EZ can then be transferred to ions in cells to create signals in cells.  Cells spend a lot of energy pumping charges (positive ions like potassium and sodium, and negative ions like chloride) through their cell membrane to make sure that inside the cell is more negative than outside.  Neurons do it the other way around to generate action potentials.

That separation of charge means that there’s always an electric field, and therefore a voltage, across the cell’s plasma membrane. It’s called the transmembrane potential, and it controls the enzymes and gates in the membrane, so the cell can be in charge of what’s moving in and out.  The state of water in sunlight sets the transmembrane potential.  Most biology books miss this idea because they did not understand the work of Gilbert Ling.

So an individual electric charge will always have an electric field around it, spreading out forever. And if you move that charge, the electric field will move with it. But the entire universe— wide field doesn’t move instantaneously – the movement travels out through the field at the speed of light. Which isn’t surprising, because bounces in electric fields are exactly what makes light. Every kind of light – from radio and visible light right through to X— rays and gamma rays.

If a charge (say an electron) moves up, the electric field moves up too – at the speed of light. If the charge moves down again, the field moves back down at the speed of light. No matter what speed the charge is moving at, its electric field will follow it at the speed of light, so it takes a tiny fraction of time for the whole field to catch up. And if you make the charge move up and down (or side to side, or back to front) in a nice steady rhythm, the electric field around it forms waves – like the proverbial ripples on a pond – moving out in every direction at the speed of light. There’s one crest for every bounce of the electron.

And that’s exactly half the story of how moving charges make electromagnetic radiation.

The other half involves the ‘magnetic’ bit. Whenever an electric field moves, it automatically creates a magnetic field that mimics its moves but at a 90 degree angle. So if the electric field is bobbing up, it’ll create a magnetic field bobbing out to the side. When the electric field bounces down, a magnetic field will bounce out to the other side.

An oscillating electric and magnetic field caused by the jiggling of an electric charge are exactly what causes the radio and microwave signals that come out of antennas. Cells use a DC current to cause their oscillations. In tech gear the AC alters the charges and causes electrons to loosen in the metal antenna.  When these electrons are dislocated, they are being forced to move side to side by the alternating current.  AC current and DC current do not cause the same oscillatory pattern and this creates a problem for cells.

In fact every electric wire that’s hooked up to AC power on Earth will give off some radio waves at the frequency of the power source – that’s why electric appliances can interfere with TV & radio signals which is why airplane mode was invented.  Cells where built around the DC power source of the sun because there is no RF or microwave radiation given off at the frequency of the power source.

A pure DC circuit doesn’t produce radio waves because it is impossible. A DC signal (or power) is unchanging, so there can be no light wave propagation going on. It is important to understand that fluctuating DC cannot exist – anything that fluctuates is actually AC.  This is fundamentally why you hear me on podcasts say that Tesla AC power grid is the worse invention mankind has ever had and few people understand why I say it.  Now you do.  The NTP toxicity study of Nov 2018 is the cherry on top of this idea.


Light alters charges.  Light knocks electrons out of tyrosine. Tyrosine acts like an antenna in cells and helps facilitate charge motions in cells where it is found.  Where does biological light come from to cause signaling?

Many studies have reported that biophotons arise from the many metabolic processes that occur within the cell (Grass et al., 2004; Tang and Dai, 2014; Salari et al., 2015; Mothersill et al., 2019; Van Wick et al., 2020; Zangari et al., 2021). The main source of biophotons is thought to be the mitochondria, where most of these metabolic reactions take place. All food was created by sunlight in photosynthestic webs.  In mitochondria, the process is reversed and light captured in food stuffs can be liberated for signaling.  In this way only, should food be thought of like a drug.  From oxidative phosphylation of food in the mitochondria, then light is liberated from the solar created foods.  For light to be created oxygen and ROS must be present.  In particular, biophotons appear to result from the process of oxidative metabolism, the excitation and subsequent relaxation to a stable state of reactive oxygen species. The biophotons are likely to be absorbed by a number of chromophores within the cell, including tyrosine and its phenolic ring, porphyrin, flavinic, and pyridinic rings, lipid chromophores, aromatic amino acids (tyrosine) and cytochrome c oxidase. The communication can span to other cells via cytonemes.

Cytonemes are thin, cellular projections that are specialized for exchange of signaling proteins between cells.

This light absorption – either by the same or neighboring (also called bystander) cells – can then lead to a change in electrical activity (Mothersill et al., 2019; Zangari et al., 2021). Microtubules are also suspected to play a role in this process, being involved in the intracellular transmission of the signal (Tang and Dai, 2014; Mothersill et al., 2019). There is a distinct delay, from the time of biophoton production to absorption, called delayed luminescence; the length of this delay provides key information about the functional quantum status of the cell (Salari et al., 2015).  The quantum status of the cell is a function of its redox potential.  Redox potential is a function of the charged ability in the cell.  It is intimately associated with the state of water production in mitochondria.

There are two striking features of biophotons in cells. First, they are emitted with a rather broad range of wavelengths, from ultraviolet to red and near infrared range (i.e., 200–950 nm). Such a broad range opens the possibility that particular wavelengths within that range are associated with different cellular reactions and different states of homeostasis (Dotta et al., 2014; Tang and Dai, 2014). Second, this self-generated light from neurons is not bright, not something that is detectable by the naked eye, nor even a relatively sensitive radiometer, but only with an ultra-sensitive light detection device, such as a photomultiplier or with a very specific histological stain (Zangari et al., 2021).

It has been estimated that the number of biophotons generated by a cell can vary anywhere between 2–200 photons/s/cm2(Tang and Dai, 2014; Salari et al., 2015). This level of emission appears to occur steadily, but the level is increased or decreased by an external stimulus for example, by man made light, or electrical stimulation, thermal or mechanical stress, the application of neurotransmitters like glutamate or the addition of an anesthetic or tetrodotoxin. It should be noted that both the biophoton intensity and wavelength can vary depending on the particular state of homeostasis (redox) of the cell. For example, there are distinct differences in both the numbers and wavelengths of biophotons evident between cancerous and non-cancerous cells (Tang and Dai, 2014; Salari et al., 2015).

Tyrosine absorbs light strongly in the 220nm-280nm range.  This matches it to water absorption spectra of light as well.  This should explain to you why solar light is imperative for diseases linked to chemicals made from tyrosine/phenylalanine.

Tyrosine contains a reactive hydroxyl group, thus making it much more likely to be involved in interactions with non protein atoms in cells.  Tyrosine can be created from phenylalanine too.   Tyrosine is an alpha-amino acid that is phenylalanine bearing a hydroxy substituent at position 4 on the phenyl ring.  Phenylalanine is an essential amino acid in humans while tyrosine is non-essential. Besides its incorporation into proteins, the only function of phenylalanine in humans is its conversion to tyrosine.  Tyrosine forms most of the stress neurotransmitters in the body.  Light stress lowers the production of these chemicals in humans.

Exposure to excessive blue light, nnEMF, or higher heteroplasmy rates is associated with calcium efflux in mitochondria.  As calcium effluxes rises it causes problems with neurotransmitter (NT) release; all NT’s need calcium ions in proper doses to release from synapses and work in neurons.  In particular, tyrosine can be metabolized to produce hormones such as thyroxine and triiodothyronine or it can be metabolized to produce neurotransmitters such as L-DOPA, dopamine, adrenaline, or noradrenaline. Tyrosine can also serve as a precursor of the pigment melanin and for the formation of Coenzyme Q10 used to shuttle electrons from cytochrome one to cytochrome 3.

The other chemicals in the matrix, like exotic atoms, can alter the dielectric values in the mitochondrial matrix because they change the overall charge inside the matrix. When we alter the dielectric values of tissues guess what interaction changes the most? Any change in a dielectric value directly alters the electromagnetic force generation capable between things in the water. It changes the scale of action.  People forget that the electromagnetic force gets stronger as the scale of action gets smaller and vice versa.  This changes the viscoelastic tensions in mitochondria and this changes how much redox power can be produced from our mitochondria.  







Hydrogen heat engine = your colony of mitochondria in you tissues.

Carnot showed us a few hundred years ago (1814) how any heat engines work.  Mitochondria are nature’s nantech hydrogen heat engine and they also obey this thereom. He showed that the best way to increase the efficiency of a heat engine was to INCREASE the difference in the temperature from the heat source (matrix) inside the engine and the exterior surroundings.

Now stop and re-read that last sentence 5 times. The matrix is filled with proteins and protons. Those proteins have a gel like liquid crystalline lattice that is piezoelectric. This is the location where the TCA cycle operates.  Mitochondria make CO2, water, and heat. Some haplotypes make more heat than others. Ask yourself why they do?

Summer is hot…….Cold Thermogenesis is best done in winter when its cold. We can artificially induce this in any season now. When the temperature difference is greatest between your matrix and the environment, your mitochondrial energy production ALWAYS improves, and your organ function benefits because ALL HEAT engines obtain higher efficiency when the SURROUNDing environment gets cooler to the mitochondria in tissues.

Now, what happens to a JET engine in a plane in OZ on the ground in summer. It is 45C on the ground and it takes off in ten minutes the same engine is at -40C at 40,000 feet in the air. Yet the Jet engine is more efficient in the subzero air than it was on the ground at the airport. Guess why? The temperature differential is HUGE. Is the temperature differential for your hydrogen heat engines greater or less in SUMMER? IN WINTER, it is far less.


Humans are now suffering unprecedented levels of chronic epigenetic diseases in younger and younger people. We have drastically changed our environment and lifestyle. To reverse or prevent epigenetic diseases we need to return to our natural environment.  Cold thermodynamics used in your colony of mitochondrial help.


Video above is now a decade old.  


Read it.  Absorb it.  If you want more juice from that same grape, watch my April 2016 webinar here on Patreon below.

There are ~65 billion neutrinos in the terahertz frequency passing through every square centimeter of space every second. Some come from the sun and some come from our mitochondria.

Did you know your cells are filled with crystals?  Some of them are “time crystals”.  Time crystals are clocks that measure the flow of entropy in a system

With this fact in mind, the notion of crystals vibrating of their own accord is seriously flawed when you have this amazing quantum vibration pounding the living crystals in plants and animals. Is the living state really like a tuning fork in a planet’s ionosphere?

Are we a dark mode plasma on the outside during daytime, and at night, are we able to enhance our glow mode state at night during sleep because we are filled with topologic insulators that make us act like a warm wet Bose-Einstein condensate?

Might these particles from the sun be the background source of electricity that runs life in chlorophyll and hemoglobin by electric or magnetic induction? The April 2016 webinar lays out my ideas on that topic.  Could this be how the solar plasma interacts with crystals in your red blood cells and heme-based proteins?

Light is captured by electrons and we do a lot of things with its energy and information quanta before we let it fall back to the ground state.  That is life’s major magic trick.

It appears Mother Nature selected amino acids that can build corkscrew proteins that work with the corkscrew light waves in terrestrial sunlight.  This appears to be an exclusive relationship and explains why artificial light outside or isolated from the solar spectrum cause signaling problems and interference in the system’s fidelity. That light has an altered charge density.  (See the RBC above)

When you realize what Mother nature is really up to with DNA, you begin to realize she codes for proteins that only operate with vibrational modes within the visible spectrum of the light of our star.  Nature abhors things that make her proteins vibrate out of tune.  Those things cause disease by altering how our cells sense time.

Hence the only configurations for protein chains compatible with what we call life are that the residues must form helical configurations.  This is why all proteins that vibrate are helical.  They are reacting to the largest charged plasma in the solar system called the heliospheric current sheet pictured below.  It also explains why DNA assumes its shape too.  The helix operates under the influence of this spiral-shaped magnetic field on the interplanetary medium from the solar wind shown below.  It appears this helical shape works with all living things affected by this magnetic sheet pictured below in the solar wind.

Do you know how it works?  Read the thread above.

ANSWER: https://www.patreon.com/posts/15497071

BITCOIN #43: Self sovereignty is at the core of BTC REGULATION and ROE & CASEY

Yesterday’s SCOTUS decision just inject chaos into society this summer. What is the lesson of this chaos? Unless you are prepared to give up something valuable you will never be able to truly change at all, because you’ll be forever in the control of things you can’t give up don’t be afraid of life’s chaos. Embrace it. What we call chaos today is just patterns of belief we haven’t recognized yet.

As long as people wait for permission to think thoughts, they’ll always be behind the curve of truth awaiting proof.

Yesterday SCOTUS decision revealed just how stupid Americans have become. It revealed they do not have a clue how the judicial system works. It revealed that they have fallen for the gaslighting and lies of politicians, media, and pop culture.

So many counterfeits lay siege to our ambitions, leaving us chasing money, power, sex, abortion, expecting to finally taste the red cherry on top of the cupcake.

It has revealed the inherent sense of lazy entitlement of multiple generations. It has shown that Americans have lost the ability to think for themselves. If you can’t think your government will take your life over.

Self-sovereignty and privacy are at the core of recent events.

Let me explain. Both Roe and Casey were dependent upon the claim that abortion is part of a right to “privacy” within the substantive due process protections of the 14th Amendment. But neither case relied upon a recognizable or legitimate due process test. I was alive in 1972 and I remember asking about what judges wrote in this case……

In 1972, Justice Blackmun posed the question and opportunity for the personhood of an unborn baby to be proven, and stated in his ruling, “If the suggestion of personhood is established, the appellant’s case, of course, collapses.”

In 1989, the ruling on Casey established personhood after 6 weeks, and removed the 14th amendment right to privacy as the ruling states that a woman is “no longer alone in her personhood.” Roe has actually been dead for 33 years! No one realized it……….because their brains have been discharged of redox by modern life.

Yesterday, Brandon and all of Washington keep referencing the loss of a constitutional right. Which is a bald-faced LIE! A Total lie… Planned Parenthood v. Casey replaced Roe’s standard of review with an undue burden standard. There never was, and never will be such a right.

Brandon said, “The court took away a right that was already recognized.” Reality responds, “Yeah, slavery was once seen as a right, too in the USA. Then it wasn’t.” That is how a constitutional republic operates chief.

But because no one actually knows the constitution WELL, nor do they reach beyond a state of laziness to read the rulings, they believe the lies as fact and operate from chosen ignorance.

The more abortion chaos is patched up with artificial peace, the worse the outcome when disruption occurs. If we apply this to abortion discussion, consider lovers who never argue about this topic and just avoid each other when irritated -vs- those who have self correcting conversations that result in more love afterwards. The discomfort of an argument is nothing compared to the fallout awaiting should the hard talks never happen. The love market can become so volatile, that it becomes unhealthy and that decision to stay or cash out is a personal one. Systems are not made stronger by stability but by infusions of chaos.

Chaos creates an opening…an opportunity. This is how the light gets in.  What is the light that got in yesterday into the abortion arena?

In 1973, Roe stole our rights and the power of our vote! LITERALLY…

People have been screaming on social media their right was taken away today by a group of unelected judges. But under Roe, those judges actually did have your rights held captive. It was a group of unelected officials, in the judicial system, which set and enforced laws…something they are not allowed to do under our constitution!

Today, they handed you back your rights and your power because now abortion can be voted on by the people at the state level.  This power is now in your hands again. The SCOTUS actually gave you a gift! But you’ve believed the propaganda and lies for so long, that you can’t even distinguish the truth from the bullshit of control.

Here’s where today exposes the laziness and entitlement of those so upset… They want someone else to guarantee their rights. They do not want to accept the responsibility to go vote and support your state legislature.

Abortion was not outlawed yesteray: “The powers not delegated to the United States by the Constitution, nor prohibited by it to the States, are reserved to the States respectively, or to the people.” 10th Amendment to the United States Constitution

As our founders intended…

Here is a link to the Supreme Court’s decision, so you can withstand the gaslighting: https://lnkd.in/grarfftG

Mockingbird media and the left want to scare you into the belief that your rights where taken away, when the reality is 180 degrees the opposite.  Now you get to choose what you want in the state you live in.

Governments lied and many unborn have died.  They died without both parents and the community at large having a say in what they believe is the best choice choice.  Voting on abortion at the state level is PRO CHOICE and pro- self soveignty.  Anyone who has read the 10th and 14th Amendment should get this.  Few have.

Moving forward, if you want a legal abortion, or do not want abortion in your state… if you don’t like the laws or outcome… Then going forward it is your fault. It is the voting that will make the difference.  Voting is a self-sovereign behavior.  If you value your privacy to choose………then you’ll get why these decisions are good for your right to privacy guaranteed under the constitution.

The right to privacy is being taken from us right now with money by AML/KYC laws.  I hate those laws and think they are a bigger infringement than any abortion law.  I have a thread on that too in these forums.


I am sad because I am watching a nation ready themselves to hand back their rights and freedoms to Washington again. They are willing to follow the politicians gaslighting them, saying they will restore their rights.  Americans are idiots.

But, if you let them do that, you’re giving them exactly what they want. CONTROL… There is a socialist, fascist-driven machine that is seeking to control the way you think, feel and act… and so far, in my adult life… I see them getting exactly what they want.

The liberal leaders in our country today are not mad because abortion laws changed, they are mad because power was returned to the people. But, you don’t realize this, because you have used them as a crutch, and become complacent in your dependency.

Americans have become lazy, they let the media inform them because they are unwilling to read, learn, and be taught. Abortion is just a symptom because again, it is the easy way out of a mistake or bad moment.

I am deeply grieving, not over Roe…. but because I am sad that America has become a nation so lazy, so entitled, so unaware….they will follow the blond into the dark, they have no courage to ask questions, and there is no leadership at the forefront who is willing to stand on convictions that value life, honor others and demand the truth.

What is the result of the Fourth Turning?  It is a society where privacy becomes a luxury good. Everything you considered a product since WW2, has now become a service that central planners will give you.

I am deeply afraid of what will be left in this nation for my kids, grandkids, and beyond. We have become a nation of total idiots…….complete idiots who cannot function unless another person, celebrity, politician, or influencer tells them what to think, feel, believe, or do.  I believe this laziness is why most won’t buy things like BTC to save their privacy and the things they value in life.  Privacy is a big right to give back to any government by a taxpayer.

I have my own morals that guide me. IDGAF what any State says. Do you know why?  When I was in third grade I read the Declaration of Independence.  Inside of it, Thomas Jefferson wrote that if any law is unjust, it is the duty of a PATRIOT to not follow it. In fact, If I don’t want to comply with a law I think is unjust, I’ll do everything in my power to find an alternative or way around it.  I reject apathy in my life.


When the world changes be ready. The SCOTUS decision just did that for you.  You might not triumph over adversity& chaos now, but you may find adversity turns into opportunity when the world finally adapts. Tailrisk matters, because extremes inform the mean.

Lives are changed with chaos infusions. What was the lesson for us all that kept resonating? Don’t let the expectations and opinions of others affect your thinking or your decisions. It’s your life, not theirs. Do what matters most to you; do what makes you feel alive and happy. Don’t let the expectations and ideas of others limit who you are.

Stop letting your past bleed into your future. If you let others tell you who you are, you are living their reality — not yours. There is more to life than pleasing people. There is much more to life than following others’ prescribed path. Build your own with unique choices for you. There is so much more to life than what you experience right now. You need to decide who you are for yourself. Become a whole being. Sculpt your life with Adventures you think of and do.

I realize it’s not easy for all people to do this, but if you can, you may want to try being self-sovereign for a change.  That is what the 4th of July is about!  This idea of self sovereignty has entered every aspect of your life in case you do not realize it.

People shouldn’t be afraid of their government. Governments should be afraid of their people!

Stop being apathetic and go vote in your state on abortion.  Do something with your freedom this 4th of July.




Life requires the optimization of light, water, and magnetism. How did magnetic forces begin to sculpt life on Earth? Where might the energy in our dynamo come from that creates the Earth’s magnetic field?

Earth and Mercury are the only planets in our system whose magnetic fields are generated by the movement of liquid metal at their cores. Mercury’s magnetic field is 100 times weaker than Earth’s. It’s billions of years old and recently discovered data suggests that it was at one point as strong as Earth’s. Of all of these natural magnets, the Earth’s magnetic field is the most important to the existence of all things living. If Earth didn’t have a magnetic field, all living things would be in trouble. The magnetic field protects us from harmful radiation from the Sun and helps keep our atmosphere from leaking into space.

The Earth behaves like a gigantic electric circuit in our solar system. The moon is the Earth’s metrnome.  The Earth’s electromagnetic field surrounds and protects all living things with a natural frequency pulsation of 7.83 hertz on average. Schumann predicted it mathematically in 1952.  That frequency is critical controlling the periodicity of clocks in living things.

How do you create the concept of a singular time if your system spans the galaxy? How do you measure time in a timeless realm? This is a question that life had to ask nature in order to exist. What was her answer to this vexing question?  The physics of organisms creates time for cells. The cellular organization of atoms in the SCN creates time using sunlight from the environment. All life on Earth gets all its energy and information from the sun. Sunlight or the photons that make up the light that falls to Earth are timeless. Light photons never experience time.  They begin to experience time when magnetism enters the fray of life.  A clock is a thermal machine that creates the illusion of time.  Magnetism in the core drives the thermal machine that create time.   The exhaust of the thermal machine is critical to see to understand the process.

Like an engine, a clock harnesses the flow of energy to do work, producing exhaust in the process. Engines use this energy to propel; and clocks use it to tick. The exhaust in living cells is codified in the CO2 and water appears via transformed atoms by mitochondrial components with the amount of heat generated. Entropy, in the form of energy or information — is the quantity whose incessant rise in the universe is closely associated with the created arrow of time.  Free radicals are the exhaust in mitochondria that drive the arrow of time in your thermal machines, called cells.  There is a deep reason mitochondria create their own magnetic field.  That field is entangled to the one in the core of the Earth to maintain life’s periodicity. Periodicity = time accuracy.  QED requires precision to maintain coherence.

A clock is anything that undergoes irreversible changes: changes in which energy spreads out among more particles or into a broader area. Energy tends to dissipate — and entropy, a measure of its dissipation, tends to increase — simply because there are far, far more ways for energy to be spread out than for it to be highly concentrated.

With this perspective, life cannot exist without a magnetic field because it limits the spectrum of the solar wind to something tolerable and it creates the conditions of existence to create a resonance cavity that envelops the planet and all living things so they connect to all the power sources the solar system supplies to Earth. Life taps all of these sources.


The isotope 4He is produced by radioactive decay in the Earth’s crust and accumulates in the same reservoirs as fossil fuels (mostly natural gas)

Helium-4 (4^He) is a stable isotope of the element helium. It is by far the more abundant of the two naturally occurring isotopes of helium, making up about 99.99986% of the helium on Earth. Its nucleus is identical to an alpha particle and consists of two protons and two neutrons.

Alpha decay of heavy elements in the Earth’s crust is the source of most naturally occurring helium-4 on Earth, produced after the planet cooled and solidified. While it is also produced by nuclear fusion in stars, most helium-4 in the Sun and in the universe is thought to have been produced by the Big Bang, and is referred to as “primordial helium”. However, primordial helium-4 is largely absent from the Earth, having escaped during the high-temperature phase of Earth’s formation.

Helium-4 makes up about one-quarter of the ordinary matter in the universe by mass, with almost all of the rest being hydrogen.

The CNO cycle (for carbon-nitrogen–oxygen) is one of the two presently known sets of fusion reactions by which stars convert hydrogen to helium, the other being the proton-proton chain reaction (p-p cycle), which is more efficient at the Sun’s core temperature. The CNO cycle is hypothesized to be dominant in stars that are more than 1.3 times as massive as the Sun.

I have a sense in the future we will discover that p-p fusion can happen on lower mass objects like planets. Planets have a lower mass and likely contain an unknown mechanism to operate fusion reactions of hydrogen and helium at lower temperatures. 

I believe the energy that creates the Earth’s dynamo comes from energy production by magnetic confinement fusion. I got this idea from reading about manufactured fusion at Princeton University long ago.  Below is a picture of how magnetic confinement fusion happens.  The Dept. of Energy has been working on this a long time.

The most well-known of the nuclear fusion test reactors is the Tokamak Fusion Test Reactor(TFTR) at Princeton. It is a magnetic confinement reactor using the toroidal geometry of the tokamak, a device first developed in the USSR. It operated at Princeton from 1982 to 1997 and made many contributions to the study of nuclear fusion. It uses a combination of two magnetic fields to confine and control the plasma. One is provided by the doughnut-shaped set of external coils which provides a magnetic field along the axis of the toroid (called the toroidal field). The other is generated by the large heating current along the toroid which heats the plasma; it is called a poloidal field. This heating current is induced by changing magnetic fields in central induction coils and exceeds a million amperes. In addition to the plasma heating by this axial current, the plasma is heated by intense beams of neutral atoms which are injected into the plasma. Below is a picture inside of the Tokamuck.

I think the collisions of two planets might have created similar conditions suitable to overcome the Coulomb force of protons to ignite a dynamo inside the planet hit.  This process would be temperature and pressure dependent fusion surrounded by a complex magnetic field of colliding toroids.

To test this hypothesis the number of neutrinos released in the reaction will be key to solving it. Why do I say this?

Neutrino production is extremely sensitive to the temperature of the fusion reaction. The proton-proton chain is more prominent in stars the mass of the Sun or less. This pp-chain reaction starts at temperatures around 4×10^6 K = 4 megakelvins = 3,999,726.85 Celcius = 7,199,540.33 F.  Could the collision of two planets provide the spark that lit the dynamo inside of Earth?  I think so.  Planetary collision fueled fusion will emit far less neutrinos than the sun.


Above = Logarithm of the relative energy output (ε) of proton-proton (p-p), CNO, and triple-α fusion processes at different temperatures (T).  Note how the green line continues downway below the sun’s temperatures and still allows for proton-proton fusion.  This is the region where I think the Earth core operates. The dashed line shows the combined energy generation of the p-p and CNO processes within a star.  This is the part of the curve where fusion has to be stellar and not planetary.  

A self-maintaining CNO chain starts at approximately 15×10^6 K, but its energy output rises much more rapidly with increasing temperatures so that it becomes the dominant source of energy at approximately 17×10^6 K.

The Sun has a core temperature of around 15.7×10^6 Kelvin and only 1.7% of

Helium 4 nuclei produced in the Sun are born in the CNO cycle.


The first reports of the experimental detection of the neutrinos produced by the CNO cycle in the Sun were published in 2020. This shows you how recent this development is.  This was also the first experimental confirmation that the Sun might use the CNO cycle.


Helium-3 (3He) is a light, stable isotope of helium with two protons and one neutron (the most common isotope, helium-4, has two protons and two neutrons in contrast). Other than protium (ordinary hydrogen), helium-3 is the only stable isotope of any element with more protons than neutrons. Helium-3 was discovered in 1939.

Helium-3 occurs as a primordial nuclide, escaping from Earth’s crust into its atmosphere and into outer space over millions of years. Helium-3 is also thought to be a natural nucleogenic and cosmogenic nuclide, one produced when lithium is bombarded by natural neutrons, which can be released by spontaneous fission and by nuclear reactions with cosmic rays. Some of the helium-3 found in the terrestrial atmosphere is also an artifact of atmospheric and underwater nuclear weapons testing.

Much speculation has been made over the possibility of helium-3 as a future energy source.Unlike most nuclear fusion reactions, the fusion of helium-3 atoms releases large amounts of energy without causing the surrounding material to become radioactive. However, the temperatures required to achieve helium-3 fusion reactions are much higher than in traditional fusion reactions

The magnetic dynamo on our planet cannot be explained by our planet’s mass. If it could the Earth, should be a dead red desert like Mars, but it remains viable and has optimized light, water, and magnetism to sustain life here for 3.8 billion years so far. 

Life needs energy to remain viable.  Much speculation has been made over the possibility of helium-3 as an ideal future energy source. Unlike most nuclear fusion reactions, the fusion of helium-3 atoms releases large amounts of energy without causing the surrounding material to become radioactive. Funny, life on Earth can tolerate some radiation just not a lot. This makes helium 3 something I am interested in.

Helium 3 is scarce on Earth because the planet’s atmosphere and magnetic field largely deflect the brunt of the solar wind, but the moon is far less protected. The only thing that’s close to the sun that has neither an atmosphere nor a magnetic field is the moon. People forget that moon and Earth have a complicated entangled history.  The video above shows that at the 4:11 mark.


The samples from the Apollo program show elevated levels of the lighter isotope of helium 3 compared to the puny amounts available on Earth. Researchers estimate that there are a million metric tons of helium 3 embedded in the outermost layer of the moon’s crust.

The small isotope difference in Helium on the moon is also found in oxygen isotopes as well. The Earth and Moon are believed to have been created in a collision that gave both an identical chemical footprint. We believed this until 2022.  It turns out their profiles aren’t identical after all because of recent studies on atmospheric Helium concentrations and fossil fuel use.  

What is more, the difference increases when you look at rocks from the Moon’s mantle, which is a layer below the surface or crust – having more lighter oxygen and helium isotopes than the Earth. This is an important lesson. The crust is where mixed debris would have ended up, whereas the deep interior would have more bits of the planet that hit us called, Theia.

Because of gravity, one should expect slightly more of the heavier isotopes closer to the Sun. Compared to Earth, Theia must have had more of the lighter oxygen isotopes, which suggests that it would have formed further away from the Sun than the Earth.

Normally, fusion is not possible on Earth because the strongly repulsive electrostatic forces between the positively charged nuclei would prevent them from getting close enough together to collide and for p-p fusion to occur.  This is called the Coulomb force.   

I have a sense that belief will be proven false some day in our future. I have a sense within the core of Earth due to our collision with Theia, there resides a real small, but strong Tesla magnetic field using a high-temperature superconducting electromagnet that powers the flow of molten metals in our core. 

What might create that in Nature? How about a massive collision between planets 4.5 billion years ago that hit the right temperature?  


The moon was created by a collision of two planets.  That is the most widely accepted theory.  It is called the giant-impact theory. It proposes that the Moon formed during a collision between the Earth and another small planet, about the size of Mars. The debris from this impact collected in an orbit around Earth to form the Moon.  This is why its orbit is circular and not an ellipse.

There is no uncertainty at all that there are huge quantities of long-lived radioactive atoms in the deep Earth. The neutrino flux from the uranium and thorium chains has been measured (by Borexino and KamLAND) as totaling around 24 TW thermal energy (out of a total of around 44 TW). Potassium radioactivity is an unmeasured but significant source. These same measurements have caused many scientists to rule out a central reactor model of the Earth, but I have a sense their calculations are dead wrong because they are missing key data.  What is that data?  The reactor inside of us is shielded by this strong magnetic field ruining the measurement ability we have today.  This is the same reason we do not know a lot about what really happens in the core of the sun right now.  I think the key to the story will be found in neutrino production by the dynamo.   

What is the clue that leads me to this conclusion?  Since 1974 the globe has been poking holes into the crust and mantle looking for hydrocarbons.  If there was a hydrogen/helium magnetic fusion device on the Earth for 4.5 billion years, poking holes in it should release a ton of helium-4 into the atmosphere when humans look for oil.  Is there any evidence for this conjecture I am laying out in this blog?  Take a look at Birner et al. 2022 paper cited below.   

Levels of helium-4 in the Earth’s atmosphere have been increasing since at least 1974.  Remember Helium is one of the rarest elements on the Earth.

What was the most interesting part of Birner’s work to me?  The very rare Helium 3 isotope is also increasing with helium 4 in our atmosphere.

That tells me there is a large source of hydrogen and helium deep in our planet for some unknown reason.   Birner is blaming anthropogenic emissions as the missing piece of the helium story.  I don’t think it is the burning of fossil fuels.  I think it is evidence of a natural source of magnetically confined fusion.  


Furthermore, the natural radioactivity of the Earth typically contributes roughly one-quarter of the basic background radiation dose that we are all getting all the time (mean is about 1 millirem per day). Potassium 40 is common in many building materials and in high potassium food such as bananas, carbon 14 is ubiquitous in the biosphere, and radon outgassing can contribute more than cosmic rays in an improperly vented structure over granite formation (which can be so deep the residents aren’t aware of them).

Inside the Sun, this process begins with protons (which are simply a lone hydrogen nucleus) and through a series of steps, these protons fuse together and are turned into helium. This fusion process occurs inside the core of the Sun, and the transformation results in a release of energy that keeps the sun hot.

It is important to note that the core is the only part of the Sun that produces any significant amount of heat through fusion (it contributes about 99%).  The rest of the Sun is heated by energy transferred outward from the core.

The overall process of proton-proton fusion within the Sun can be broken down into several simple steps. A visual representation of this process is shown in Figure 1 below.   I believe our core inside of Earth is running proton-proton fusion at low temperatures and it is magnetically confined because of our collision with Theia.

Now you know why there is a space race to the South Pole of the moon by China and the USA.  Now you know why Musk is favored by our government.  Now you know why we need to build a moon base like the one pictured above.

The steps are as follows:

Two protons within the Sun fuse. Most of the time the pair breaks apart again, but sometimes one of the protons transforms into a neutron via the weak nuclear force. Along with the transformation into a neutron, a positron and neutrino are formed. This resulting proton-neutron pair that forms sometimes is known as deuterium.  Deuterium is the heavier isotope of hydrogen.

A third proton collides with the formed deuterium. This collision results in the formation of a helium-3 nucleus and a gamma-ray. These gamma rays work their way out from the core of the Sun and are released as sunlight.  On Earth, I believe these are confined by the magnetic confinement of our flowing molten core and are being used to drive the core.  I think helium is leaking slowly over billions of years into the hydrocarbon basins created by extinct life over billions of years that make up oil basins. Humans are the first species that evolved on Earth and can tap the Earth to get to the two helium isotopes made in the core.

Two helium-3 nuclei collide, creating a helium-4 nucleus plus two extra protons that escape as two hydrogens. Technically, beryllium-6 nuclei form first but are unstable and thus disintegrate into the helium-4 nucleus.  I am not sure that this step happens in the core of Earth because of our lower temperature barrier.  I think this is why the Earth is leeching slow amounts of Helium 3 and 4 into the mantle.  In fact, I would bet our planet’s core has a massive amount of beryllium in its flowing magma that would be a fingerprint for the fusion event I am describing to you.  


The final helium-4 atom has less mass than the original 4 protons that came together (see E=mc^2). Because of this, their combination results in an excess of energy being released in the form of heat and light that exits the Sun, given by the mass-energy equivalence. To exit the Sun, this energy must travel through many layers to the photosphere before it can actually emerge into space as sunlight. Magnetic confinement in the Earth’s core would keep the energy confined to keep the core molten to drive the tectonic plate movements on the surface.

If you want to understand the power of helium fusion consider this:

Assume that the average continental crust weighs in at about 10 cubic feet to the ton. If a ton equals 2000 pounds, this means that each cubic foot of continental crust weighs about 200 pounds. How big is North America?

Since we’re just trying to get an “order of magnitude” number here, let’s assume that on average it’s approximately 2500 miles from east to west, 5000 miles from north to south, and 35 miles thick. Let’s see here now: converting to feet that make 1.3 X 10^7 feet times 2.6 X 10^7 feet times 35 feet which equals 1.2 X 10^16 cubic feet, times 200 pounds equals 2.4 X 10^18 pounds. In normal numbers this is the same as 2,400,000,000,000,000,000 pounds (2.4 quintillion). What power source can do this?

With this much mass, we can start to rule out some possibilities. The gravitational attraction of the moon just doesn’t do the job. Nor does the attraction of the sun. The centrifugal force from the rotation of the earth probably can’t get it done.  What does it leave?

Probably the most logical place to look is inside the earth. We already know that it’s pretty hot down there, and we also know that heat and density are related to physics. The short version is that when something is heated up, there is a corresponding decrease in density, and the material rises to where hydrocarbons would be in extinct carbon basins. This is the reason hot air balloons work, why the cold water is near the bottom of the lake and not on top, and why helium 3 and 4 are in hydrocarbon basins.

This process also drives the major wind patterns. Rock is no different, and when heated it lowers in density and wants to go up. So far so good. The problem is that if it rises it’s going to leave a void where it was, and we sure can’t have that. Just like in the lake (or the atmosphere), water, air, helium isotopes, or in this case rock, moves in from the side to fill the hole. But that just leaves another hole, so something has to move in to fill that one, and so on and so on until the stuff which moved in the first place do the filling and the circle is complete.

We call this circular pattern of density-driven material a “convection cell,” and as I said it’s this convection that powers the major global wind patterns, affects the ocean currents… and likely drives the tectonic plates on our planet. Deep beneath the crust the rock is VERY hot, and while there is probably too much pressure for it to be a liquid, it’s still somewhat mobile, and individual atoms like Helium and such can kinda/sorta ooze about, setting up convection cells which may carry the plates along where they rub up against the surface crust.  This is how helium isotopes move too.

Most geologists accept convection currents as the most likely mechanism for plate motions. One of the biggest questions now relates to how deep within the mantle the convection cells extend.

Birner doesn’t seem to see the connections I do.  I just entangled with him on Clubhouse a few days ago to give him a clue to look deeper before pointing to climate change.  I did this in a group called Quantum Photonics.  If you are crafty enough you probably can find the replay there.  Or maybe, he reads this post because someone sent it to him.

Since this proton-proton chain happens frequently – 9.2 x 10^37 times per second – there is a significant release of energy. The core will run at far lower temperatures.  Of all of the mass that undergoes this fusion process, only about 0.7% of it is turned into energy. Although this seems like a small amount of mass in the sun, this is equal to 4.26 million metric tonnes of matter being converted to energy per second. In Earth, this conversion means our core should burn 22 billion years moving the tectonic plates above.  In other words, the core will be here longer than the sun will.  The sun is expected to become a red giant and swallow Earth in about 10-12 billion years.  In the sun, using the mass-energy equivalence, we find that this 4.26 million metric tonnes of the matter are equal to about 3.8 x 10^26 joules of energy released per second!


ITER (initially the International Thermonuclear Experimental Reactor, iter meaning “the way” or “the path” in Latin) is international nuclear fusion research and engineering megaproject aimed at replicating the fusion processes of the Sun to create energy on the Earth.  


How does this story of the creation of our magnetic field scale to your life right now? Your worldview has to be structured in principle on some specific doctrine that shapes how you function and view humanity.  Embracing Quantum Electrodynamic theory in biology is akin to wearing steel-toed boots in a ballet-slipper world.  Understanding that life is bigger than your set of challenges will help you overcome obstacles that will come your way from time to time.

How does all this fancy physics begin to make sense in your biology?

Protein modification is of major interest to a quantum biologist.  All proteins are hydrated and their chemical structures act as light antennae for incident solar EMFs.  When different incident light waves are present, post-translational modifications are induced or become necessary to maintain physiologic functioning.  Recall that the incident light wave is electromagnetic.  When it is absorbed by a protein or its side change it is changed into a specific type of electro-mechanical wave that is used by the hydration shell in the cell to signal a variety of different events.

Here is a list of some of those events and what they do for a cell.  Indeed, many intra- and extracellular events depend on an occurrence of a specific chemical change that drives the change in both protein structure and function. These chemical modifications are commonly referred to as posttranslational modifications (PTM’s), as they occur after the protein biosynthesis step, i.e., the translation. PTMs and proteins involved in mediating their incorporation into target proteins add additional layers to functional properties and diversities in the proteome and are the key to a number of crucial biological processes. For example, prior to degradation, proteins are often modified several times, leading to profound variation in their behavior.

In general, the incorporation of PTMs takes advantage of the chemical reactivity of the amino acid side chains and leads to specific functional outcomes. Upon phosphorylation (addition of a phosphate group to the side chain hydroxyl group of a serine, threonine, and tyrosine residue), conformational switches (de)activate protein-protein interactions and downstream events; upon farnesylation (addition of a farnesyl group to the side chain thio group of a cysteine residue), proteins get translocated to the membrane; and upon ubiquitination (addition of a small protein, ubiquitin, to the side chain amino group of a lysine residue), proteins are recruited by the 26S proteasome for degradation.  I have an entire blog series on this one process because it is a critically important step in oncogenesis.  Proteins can also undergo glycosylation, the addition of saccharide units; acetylation, the addition of acetyl groups to the side chain amino group of a lysine residue; formylation, in which a formyl group is added to the N terminus of a protein; amidation, in which a formyl group is added at the protein C terminus; sumoylation, the addition of a small protein, SUMO, to the side chain amino group of a lysine residue; and biotinylation, the addition of a biotin molecule, to mention only a few.

Light from our native environment programs the things inside a cell to do all these amazing post-translational modifications.  The magnetic field of the Earth assists light in this process by getting Nature’s recipes perfected.  It helps craft the Schumann resonance which increases the periodicity of the molecular clocks in cells to coordinate all these modifications.  The higher periodicity of a clock correlates to its accuracy.  QED requires precision to maintain coherence in the living state.  It has been done using a quantum mechanical method of chronic testing done over 4 billion years inside of every cell in your body.  It has done this in ever cell that has ever existed on this planet.

Overall, it’s fair to say that selective modification of proteins is a key step in most biological processes. Nature uses a covalent modification of proteins to modulate their function. We call this process “evolution”.  I call it “change without much changing”, except light frequencies. As such, many natural products, originating from millions of years of evolution, have adapted their structure for covalent binding to proteins.  Light is what sculpts the semiconductors of life, in my humble opinion.  Proteins are those semiconductors.  The evolutionary process toward life all began with a planetary collision.  Now you can see just how important magnetism is to all of us.   (Drahl et al., 2005; Pucheault, 2008).






So in many of my podcasts,  I taught you about how the loss of negative feedback control in coupled biologic systems is the sentinel event for aging and disease generation.  When one side of a coupled system is lost the result with be extinction of both the positive and negative feedback loop.  This is why taking oral melatonin can lead to blindness by thinning of your retina.  It was also the reasons removal of the wolf from Yellowstone Park caused the topology of the rivers to change and cause many other animals to become extinct in the park.

I used the predator or prey in this analogy to make the point of how decentralization maintains control of feedback loops. If you alter the balance of predator or prey the result is always the EXTINCTION of both preadtor and prey. I have told you that in aging and neolithic disease generation NAD+ becomes altered in relation to the level of NADH. This can happen by several stimuli from the environment.  NAD+ and NADH operate just like predator and prey within the circadian mechanism.  If you get the light in your environment wrong you will destroy both NAD+ and NADH and you will never be able to control where electrons and protons are needed in cells.  If you disrupt NAD+ your circadian clocks can no longer OPERATE.

^^^^This will become important when you review the end of this blog carefully.


It is how mammals capture electrons and protons from foods.

NAD+ serves as a crucial determinant of the abundance of other species of NAD such as the reduced form of NAD phosphate (NADP(H)). Alongside NAD(H), NADP(H) pools play crucial roles in REDOX maintenance, particularly as antioxidant cofactors (reviewed in Ying, 2008 and Xiao et al., 2018).  How it is destroyed or made inside a cell is one of the best measures of how the redox potential varies between the creative and destructive cycles in a decentralized fashion.

PARPs are seen as one of the dominant enzymatic consumers of NAD+ within the cell.  Humans have 17 types of PARPs.  One of the 17 is called PPAR alpha.  It is the master regulator of fat-burning in mitochondria.  PPAR alpha upregulates CPT1, which controls the rate at which fat enters the mitochondria.  The rate at the entrance must marry to the timing of oxidation in the system to be burned properly.  Timing is critical in the ledger of life.

You must have reserved or created 3 NAD+ to ride the fat-burning train to longevity.  Without it, you lose LIFE -time = longevity

PPARα, a transcription factor that modulates fatty acid metabolism, regulates substrate preference in organs with a high density of mitochondria.  (heart/brain/bone/immune system)

Three pathways of NAD+ biosynthesis within mammals have been identified: #1 is the Salvage pathway, #2 is the de novo, and #3 is the Preiss-handler pathway.

During basal conditions of diurnal life, the salvage pathway is currently believed to be the dominant source of NAD+.  In recent times, evidence has been presented that all 3 NAD+ biosynthesis pathways can switch between (Zhang et al., 2019) and compensate for one another (Okabe et al., 2019) in mammals.

The de novo and Preiss-handler pathways are dependent on dietary derived vitamin B3 precursors.

The salvage pathway seems to be most affected by the light and dark cycles of circadian biology.  The de novo pathway is also called the kynurenine metabolic pathway.  I’ve written about it in time crystal blogs in the quantum thermodynamic series here on Patreon.  The Preiss-handler pathway utilizes nicotinic acid (NA).

The chronic loss of NAD+ is the critical sign of a loss of negative feedback control of the ubiquitin cycle when there is a light (photon) mismatch in the animal’s environment. When this occurs the inner mitochondrial membrane does not oscillate at 100 Hz, fat burning doesn’t operate well, and there is no alignment of the mitochondrion’s IMJ’s as seen below.  Our colony of mitochondria use this information to alter the rate of fat oxidation from winter to summer.  The sun informs the colony of mitochondria when to do this using charge and angular momentum of electrons and protons stripped from foods.

What does this imply if we eat outside the seasonal photosynethic windows or under artificial light?  The mitochondria engine can become easily flooded with electrons and protons.  A flooded engine is an internal combustion engine that has been fed an excessively rich air-fuel mixture that cannot be ignited.  When a combustion engine gets flooded in this way an engine would make a tell-tale bogging sound and black smoke would come out of the tailpipe.  The black smoke also alters the ROS in the system.  Is there a clue in our blood that ROS is spiking inside the mitochondria?  Yes, there is.

The problem with the flooded engine is too much fuel (electrons/protons and not enough oxygen = ROS drops.  This is why diabetics have no superoxide pulse at cytochrome 1.

NAD+ is what captures electrons and protons in mitochondria.  If you are diabetic can you capture electrons or protons well?

Electrons and protons are what sculpts the matter in cells.  Many people in biology think that only DNA can sculpt atoms to create life.  They always forget DNA only code for amino acids that create proteins.  There is another way we sculpt matter using NAD+.  NAD+ is how we get theses chiesels.

NAD+ changes in relation to the electromagnetic spectrum of light in a person’s environment while they act to cause evolutionary changes via redox management.  How does this happen?

Angular momentum & charge are two conserved factors quantum mechanically that continue to confuse biologic scientists. If biology realized that the addition or subtraction of electrons and protons could change the solid-state function of proteins they’d realize finally why we do not need DNA/RNA changes to explain the small human genome.  The implications of this are massive and largely unknown in biology.  It means that the syntax of genes is vastly more complex than Darwinist believe.  It is more subtle and nuanced than any spoken language or genetic language known to man today.  The reason this is the case, is that genes themselves can be changed by alterations of the angular momentum and charges as electrons and protons move due to solar frequencies.  

DNA only codes for proteins and nothing else. DNA/RNA main purpose is to create a solid-state semiconductor that operates with the light of our star. The light of our star is the optimized electromagnetic signals mitochondria operate with.  Anything OTHER part of the electromagnetic spectrum changes angular momentum and charge and reduces the fidelity of information processing in our cells paving the way for disease propagation. NAD+/NADH couple respond to the change in light because they capture electrons and protons from hydrogen molecules in foods.  The type of hydrogen is critical in the physiologic function of NAD+/NADH in a cell.  If a cell is forced to deal with too much deuterium NAD+/NADH won’t have many electrons and protons to capture.  That is a low energy state. That is what artificial light and artificial food cause in mitochondria.

This lack of electrons and protons manifests via mitochondrial dysfunction. Acylcarnitines play an essential role in regulating the balance of intracellular sugar and lipid metabolism. They serve as carriers to transport activated long-chain fatty acids into mitochondria for β-oxidation as a major source of energy for cell activities = Dx mtDNA defects. No artificial light device (PBM/PEMF/UV) device has solved this issue.  The sun is the only answer that is APPROPRIATE in optimizing NAD+ function with the correct isotope of hydrogen stripped off of foods.

Acylcarnitines are the black smoke created by a flooded mitochondrial engine in cells.

A metabolic hallmark of mitochondrial diseases like obesity and diabetes is high circulating levels of acylcarnitines.
The enzyme that controls fat flow into the mitochondria is called carnitine palmitoyltransferase (CPT1).  This enzyme takes a free fatty acid (palmitate) and transfers it (that’s the transferase part) to a chaperone molecule called carnitine.  Free fatty acids contain an acyl group on one end, so a molecule of fat attached to carnitine is an acylcarnitine.

If you don’t care to memorize all of that, just remember that acylcarnitines are unburnt fuel.  Once a fat is transferred to carnitine, it is supposed to be sent into the mitochondria to be burned (oxidized) by the TCA cycle.

Oxidative balance controls the metabolic rate but it DOES NOT define the redox state of the cell.  The level of ROS/RNS does.  Where the ROS comes from also matters deeply in this time ledger.


Once inside the mitochondria, the acyl group is transferred from carnitine to another chaperone molecule called Coenzyme A (CoA) to become acyl-CoA.  Fats are broken down in a process called beta-oxidation.  Every round of beta-oxidation produces an acetyl-CoA and a shortened acyl-CoA.  Most fats are 16 or 18 carbons in length and an acetyl group has two carbons so it takes 8 or 9 rounds of beta-oxidation to turn a fat all of the way into acetyl-CoA.  One molecule of fat makes 8 or 9 acetyl-CoA, each of which takes 3 NAD+ to be fully burned.

NAD+ is needed to move the fatty acyl-CoA past the hydroxyacyl-CoA step.


The intrinsic value of vitamin B3-derived NAD+ to human health leads to hyper photosensitivity to sunlight.  This is why so many are solar sensitive or are told they are “allergic” to the sun.  This so-called allergy to the sun is linked to the simultaneous reduction of NAD+ and melatonin due to a lack of sunlight exposure during the day or too much artificial light at night or a combination of both.  They are deficient in NAD+ while having a horrendous redox. Low redox = low energy = low solar exposure state

Most of these people have atrophic skins and downregulated melanin production. Everyone with a melanin issue on their skin gas an altered NAD+ level in their mitochondria.  The reduction of melatonin has direct mitochondrial effects.  Melatonin optimizes autophagy and apoptosis in our colony of mitochondria.  This means melatonin optimizes fat metabolism by controlling heteroplasmy state in mtDNA. (below).  Certain seasons fat metabolism operates better.  Sunlight and temperature controls this “thermostat” in mitochondria.

Melatonin is the chemical in non-hibernating mammals that simulate torpor. Torpor is the metabolic state that mammals use to lower their body temperature to hibernate.

Melatonin acts to lower our thermostat in our hypothalamus at night time after 4 hours of darkness to lower the temperature of CSF around our brain. This allows the passage of leptin into the hypothalamus and removes the need for electrons from food (helps a low NAD+ state).  This is how animals live off their fat stores during sleep of any duration.  

This is why the leptin Rx uses protein early in the day to offset the inability to burn fats well.  Protein satiates animals quickest irrespective of their mitochondrial status.  Eating a lot of protein is not easy to do so.   It also lowers food intake, as a consequence.  

The effect of fasting during hibernation or sleep in mammals causes a rapid rise in PPAR alpha – the master regulator of fat burning because during these times subcutaneous fat is the only source of electrons available for mitochondria.  PPAR alpha upregulates CPT1, which I’m sure you remember is the enzyme that controls the rate at which fat enters the mitochondria.

Sleeping/torpid animals are in reductive stress because they have highly acetylated mitochondrial enzymes.

The sirtuin proteins perform this task and this is why taking sirtuins during the day makes no quantum mechanical sense.  When animals are sleeping or want to get out of torpor, they surge the production of sirtuin deacetylases to allow mitochondria to operate fully.

All that you have to do to induce torpor is to flood the mitochondria with fat.  This is why the Leptin Rx does not use a high-fat diet.  Fat is very rich in acetyl groups, providing three times as many, gram per gram, like glucose.  The surge of acetyl-CoA runs down NAD+ levels at cytochrome 1 and floods their little engines = acetylcarnitine rises in the blood.

There is a catch because not all fat types induce sleep/torpor equally.  Mammals fed saturated fatcontinued to burn more oxygen compared to the PUFA fed mammals, maintaining a higher metabolic rate.  H+ speeds your metabolic rate up and deuterium tends to slow it down because of its effects on NAD+.  This modulated by your thyroid hormones.   Saturated fats have the highest amount of H+ in them and the lowest amount deuterium in them.  Deuterium does not liberate as many electrons or protons to NAD+ due to its kinetic isotope effect so it becomes an option that mitochondria can use to limit overfilling the engine with protons and electrons as light varies during the seasons.


Now for how this scales to your molecular circadian clock and your peripheral clock genes (CCG’s). The current model of the mammalian circadian clock includes two interlocking transcription-translation feedback loops comprised of several so-called “clock” genes and their protein products, which ultimately regulate the transcription of “clock-controlled” genes.  Melatonin receptors (MT1,2) are critical in this timing mechanism.


These feedback loops consist of positive and negative components. The positive components include the basic helix-loop-helix-PAS domain transcription factors, CLOCK, and BMAL1. These transcription factors heterodimerize, translocate from the cytosol to the nucleus, and bind to circadian E-box promoter elements that enhance the transcription of genes encoding the negative components PERIOD 1 & 2 and CRYPTOCHROME 1 & 2. The CRYPTOCHROME and PERIOD proteins feedback inhibit the transcription of the Cryptochrome and Period genes by blocking CLOCK/BMAL1-mediated trans-activation.

The second feedback loop involves the trans-activation of the Rev-Erbα and Rora genes by CLOCK/BMAL1. The protein products of these genes compete for binding to RRE elements in the Bmal1 promoter, driving a daily rhythm of Bmal1 transcription and closing the second feedback loop. Rhythmic expression of these clock gene products produces circadian clock outputs by regulating the transcription of clock-controlled genes (CCGs).

Remember melatonin is made from tryptophan.  So is NAD+ as I laid out in the Time crystal blog.

Seasonal sources of electrons and protons in foods varies via the sunlight used in the photosynthetic process used to create them in Nature.  NAD+ pays attention to the quality of electrons and protons and we can see this if we understand the seasonal link between acylcarnitine and the isotopes of hydrogen in foods.  Electrons will vary in the power of photons they are excited by.

In circadian biology, the electrons and protons sent to mitochondria inform the mitochondria what to do with the fuels they get.

At least some of these CCGs, including aanat, the gene encoding the penultimate enzyme in the melatonin biosynthetic pathway, contain circadian E boxes, which have a core nucleotide sequence of CACGTG and are activated rhythmically by CLOCK/BMAL1.

Post-translational regulation, including phosphorylation, acetylation (SIRT), ubiquitination, sumoylation, and proteasomal degradation is also important in the regulatory mechanisms generating the circadian oscillation to alter clock periodicity.  Clocks become more accurate the higher periodicity they have.  Seasonal light alters circadian periodicty of clock genes.

Once your SCN goes haywire in your eye, it is a matter of time before your circadian clock genes in tissues the SCN controls go haywire and malfunction and lead to disease. What will be the ultimate result? EXTINCTION of both sides of the circadian coupling.

What gets extinguished?

NAD+ does.  Now you know what low melatonin really means to longevity.  If you cannot capture electrons and protons optimally in a season, you cannot ideally sculpt your mitochondrion or cells.  This is how disease manifest.


Your eye can be a clock or a camera. A blind man’s world is bounded by the limits of his touch and he relies on his timing; an ignorant man’s world by the limits of his wisdom; a successful man’s world by the limits of his vision and sense of timing.


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2. Herzog ED. Neurons and networks in daily rhythms. Nat Rev Neurosci. 2007;8:790–802.

3. Yamazaki S, Numano R, Abe M, Hida A, Takahashi R, et al. Resetting central and peripheral circadian oscillators in transgenic rats. Science. 2000;288:682–685.

4. Ko CH, Takahashi JC. Molecular components of the mammalian circadian clock. Hum Mol Genet. 2006;2:R271–277.

5. Munoz E, Baler R. The circadian E-box: when perfect is not good enough. Chronobiol Int. 2003;20:371–88.

6. Gatfield D, Schibler U. Proteasomes keep the circadian clock ticking. Science. 2007;316:1135–1136.

7. https://www.sciencedirect.com/science/article/pii/S0163782721000333


Did you know that T cells kill cells with immune synapse, within 10 minutes inter-digitated contact with actin in target cells?  Moreover, within an hour they form large tight connections, causing membrane tightens forms cluster in 2 minutes?  Did you know the centrosome directs microtubules actions in cells and moves in shoots toxic granules in six minutes in your immune system?

Why are we built like this?   What is the key reason microtubules are the key to information transfer?

The first one should be obvious.  All microtubules are nanoscopic tubes that can be filled with water.  We’ve know for years that when water is confined below 1.4 nanometers it becomes capable fo quantum mechanical behavior.  Living H2O is the water that constitutes ~70 % of cells and organisms, and without which life is impossible. Living H2O covers the surfaces of macromolecules like microtubules and membranes in cells, and interweaves with molecular fibrils of collagen and other extracellular proteins, providing intercommunication channels throughout the body so each molecule can keep in touch with every other in the ‘quantum jazz’ of life. It shapes and softens macromolecules, so they can function as coherent quantum molecular machines that transform energy at close to 100 % efficiency. Living H2O turns the whole organism liquid crystalline because it is liquid crystalline and quantum coherent. That’s why all organisms have a dancing rainbow inside when looked at under a diffraction light microscope.



Last and definitely not least, water provides the electrons and protons to fuel the photosynthesis-respiration dynamo that spins inanimate molecules into living organisms out of pure sunlight. Water is truly the medium, message and means of life.

Consider our vision.  Many of the photoreceptors in our eye have microtubules in them as you saw in the video above and the picture above.  What do we know about how vision operates today?  Even today there is the great mystery of how human vision operates:  Vivid pictures of the world appear before our mind’s eye, yet the brain’s visual system receives very little information from the world itself to see. Much of what we “see” we conjure in our heads.  A lot of the things you think you see you’re actually making up in a quantum reconstruction in your brain.  How does it happen?

Microtubules seem to be key to these abilities.


T cells activate to become killer cells and then attack infected cells and cancer with remarkable ferocity. This seems to happen magically.  When we use the term magical, you can bet a quantum mechanical process is operational behind the scenes.  This includes an ability to dramatically change its metabolism in many ways to alter its shape, speed of reproduction and ability to survive in any environment, even without oxygen.

How does a cell capture information from the environment to alter its physiological behavior?

Global cooling seems to be associated with increases in geomagnetic field intensity whereas global warming is associated with decreased geomagnetic field intensity. It appears magnetic fields changes in our environments determine how CO2 is handled in the atmosphere and seas.  This information appears to be captured in water networks in the body and transmitted to our cells via microtubule formation.

Since mitochondria make CO2 from oxidative metabolism, what might the effect be on mitochondrial function during an infection in the body?

In the human body, carbon dioxide is formed from the metabolism of carbohydrates, fats, and amino acids, in a process known as cellular respiration which occurs in mitochondria. While cellular respiration is notable for being a source of ATP, it also generates the waste product, CO2. The body gets rid of excess CO2 by breathing it out via the lungs and trachea which have abundant cilia and microtubules. However, CO2 in its normal range from 38 to 42 mm Hg plays various roles in the human body. We have chemoreceptors that pay attention to CO2 levels.  They regulate the pH of blood, stimulates breathing, and influences the affinity hemoglobin has for oxygen (O2). Fluctuations in CO2 levels are highly regulated and can cause disturbances in the human body if normal levels are not maintained.

CO2 retention is known as hypercapnia. Hypercapnia is usually due to hypoventilation or increased dead space in which the alveoli are ventilated but not perfused. The microtubules in those poorly perfused alveoli collect information from the cytoarchecture and deliver the information in quantum mechanical fashion via water networks linked to the tensgrity system in a cell’s microarchitecture.

In a state of hypercapnia or hypoventilation, there is an accumulation of CO2 in the blood. The increased CO2 causes a drop in pH, leading to a state of respiratory acidosis. The chemoreceptor reflex is important in allowing the body to respond to changes in pO2, pCO2, and pH. Chemoreceptors can be categorized as peripheral or central. This links directly to how CSF flows around the vascular in the CNS. Peripheral chemoreceptors are positioned in the carotid and aortic bodies and in the brain’s blood vessels. Central chemoreceptors are located near the ventrolateral surfaces of the medulla. While peripheral chemoreceptors are sensitive to changes in mostly O2 and CO2 and pH to a lesser degree, central chemoreceptors are sensitive to changes in pCO2 and pH.

The glomus cells in the carotid and aortic bodies detect states of hypoxia, hypercapnia, and acidosis. On the other hand, central chemoreceptors do not detect states of hypoxia. They detect a change in PCO2 very rapidly because CO2 diffuses through the blood-brain barrier (BBB) and into the CSF easily where a massive array of microtubules are present.

On the other hand, central chemoreceptors take longer to detect a change in arterial pH because H+ does not cross the BBB. When a state of hypercapnia is introduced, central chemoreceptor activity is increased. As a result, the sympathetic outflow to the vasculature is increased via the brainstem nuclei, and efforts are made to increase the respiratory rate.


The magnetic-field effect on CO2 solubility in humans is twice as large, therefore a geomagnetic field variation on Earth can modulate the carbon exchange between atmosphere and ocean.  Your microtubules can and do sense that change.   A 1% reduction in magnetic dipole moment may release up to ten times more CO2 from the surface ocean than is emitted by subaerial volcanism. This implies it does it in your body as well.  How might this affect mitochondrial function in your immune cells given what biology has found out about CO2 physiology?

Most do not know that T cells are inherently magnetic because of the amount of ferritin (iron) they contain. This is why theses cells become “magnetically frozen” to pathogens EMF signals that they react too. This is done via molecular resonance.  This action magnetically locks them into their target pathogen and the fever reaction in the hyporthalamus results and this leads to better T cell killing of the invader pathogen.  UV solar exposure unlocks the T cells magnetic grip and allows the cells to limit the cytotoxic damage to the hosts organs.

Note, most viral deaths have been in immunocompromised humans which were tied to uncontrollable cytotoxic storms causing organ destruction.  In other words, their own immune cells caused an unrelenting hurricane of damage to organs.   Also recall that most deaths in the last two years are linked to humans with significantly lowered Vitamin D levels. Note, vitamin D in cells is only made from UV light exposure of the skin.  The skin also has a massive microtubule array with deep connections to the tensgrity system of the organism. Microtubules seem to deliver the information in our environment to our skin to inform our immune cells how to operate throughout the body.

Can T cells work well on a planet with competing magnetic field signals? It appears they cannot operate properly.


A major T cell tactic is direct contact with an offending cell by forming a synapse between the two cells. This immune synapse is sometimes called a cytolytic synapse, meaning killing of a cell. Mechanisms at this synapse are very complex and involve rapid elaborate remodeling of the scaffolding inside the cell. Most of these involve microtubules which have been implicated to be one of the mechanisms Nature uses to inject quantum mechanically operations to cells.

Microtubule proteins are able to produce electromagnetic fields and have been shown to play an important role in memory formation, and learning in various cell lines. Therefore, microtubules have the potential to be affected by exogenous electromagnetic fields.

Despite very brief contact times, microtubules and actin in both cells undergo many different alterations. Structures are built with scaffolding molecules to rapidly form a temporary connection and then a very secure connection that allows multiple rapid actions. In fact, unlike other types of synapses, centrosomes are brought right up to the membrane to direct the action. Centrosomes are vital structures that coordinate all microtubule structures as well as the spindles in cell division.  They organize microtubules in the cell and I believe this is done topographically via electric and magnetic fields that map out the body plan of the organism.  Robert O. Becker was the first researcher to link electric and magnetic field polarization to body plan construction during his wound healing experiments.

Centrosomes are composed of two centrioles arranged in an orthogonal configuration, is an indispensable cellular organelle for mitosis. 130 years after its discovery, the structural-functional relationship of centrosome is still obscure.  We have clues in the literature that the centrosome might act as an electromagnetic generator in cells to direct energy and information transfer. (below)

Centrosomes are known to coordinate complex activity such as cell division, where they drag two sets of chromosomes in different directions to form two daughter cells. Centrosomes are also used to build and coordinate the microtubule highways that provide very elaborate transport along the long neuronal axon in humans.  You can see this in the cochlea and in the rod photoreceptors in the eye. The only other time that a centrosome is directly at a cell’s surface is when cilia are formed. Cilia provide both movement and the extremely elaborate signaling machine called the primary cilium. Cilia line many organs where fluid must travel, such as the secretions in the lung and the cerebrospinal fluid in the brain.

Killer T cells come from CD8+ T cells, which are originally small and quiet cells that travel about looking for problems. When they see a problem molecule in the groove on the surface of the presenting cell, they stop at the cell. This molecule from inside the cell is placed in the groove so the T cell will know if the cell is normal or infected. It is called a MHC or major histocompatibility antigen.  If it is abnormal or infected it the molecule integrin is stimulated to stick out from the T cells to grab onto the other cell. Activation produces a dramatic change in the status of the T cell that produces an army of killer cells over several days with many granules filled with molecules that are weapons. Some of these granule toxins cut holes in cells (perforin) and some (granzymes) cut proteins in cells leading to cell death. Killer cells become much bigger and develop a very complex internal architecture with scaffolding molecules.

Upon electromagnetic induction activation, a large activation cluster is formed right at the synapse, called central cSMAC (or supra molecular activation cluster). This cluster includes many special receptor molecules and a complex large machine called the microtubule-organizing center (or MTOC). MTOC is a type of centrosome where the minus ends of microtubules are anchored and from which the plus ends of microtubules extend.

Microtubules appear to be self-assembled linear hollow circular tubes with inner and outer diameters of 17 and 25 nm, respectively, growing from the centrosome in the center of the cell towards its membrane.  I believe the cSMAC and MTOC are electric generators that actually cause microtubule assembly via the electromagnetic force.

Cells can contain multiple MTOCs wherever microtubules are being used. Another cluster is formed called distal dSMAC, which is away from the synapse at the back of the cell. These two clusters work together in the processes that occur.  This appears to be how immune cells are transfering information in the environment to cells.  I believe they are using electromagnetic spectrum to convey this message.

Why do I believe this.  I covered this in my Quantum Brain blog years ago.  The work of Frolich is critical in this prediction.

The cellular electromagnetic field should propagate to all parts of the biological system.  the centrosome is key in this action.  It has to be coherent (the same frequencies, form, and phase) within the specific region: in the cell, in the tissue, and in the whole biological system. Coherence in time is also an important condition for this to happen.  Proper circadian timing makes this possible.   If time keeping is innaccurate quantum coherent mechanisms become impossible.

Oscillations of different generating ‘antennae’ must be controlled by signals delayed by one or more periods of oscillations. The cellular electromagnetic field should be generated by energy-supplied structures which are distributed inside the cell with a convenient density, are of linear geometry resembling macroscopic antenna systems.  Moreover, they should be electrically polar to react to electric fields. The generating system must be strongly nonlinear for spectral energy transfer.  Why?  Fröhlich predicted this would be a REQUIREMENT FOR the living state. Based on these assumptions, microtubules have been predicted as generators of coherent vibrations and electromagnetic field.  Most recently this was done by Pokorný et al.

The synapse first forms in the CD8 T cell and then is altered as the cell becomes a cytotoxic killer cell. At first it helps with the changeover to killer cells. In the killer cell, it is prepared to send the attack granules within minutes.

Some have speculated that microtubules form a quantum computer that directs cellular activity in the immune system. While there is no proof of this, it is interesting that many extremely important and vastly complex activities that use microtubule machines, centrosomes and spindles seem to be heavily involved in information processing in cells. This includes transport along the axon, spindles for cell division, primary cilium and moving cilia. There is no doubt that microtubules appear to operate as an intelligent LEGO like system vital to the life of many cells.


Biological activity is conditioned by a continuous energy/information supply and transformation, system ordering at various length scales, controlled processes including chemical reactions, and a massive information transfer. Microtubules seems to be at this nexus.  All these abilities life contains cannot be facilitated purely by diffusion or chemical interactions acting at the length scale of several nm as we are taught in a biochemistry book. A fast, efficient physical mechanism acting at large length scales should be involved.  This is the scale of the electromagnetic force.

Biological systems SHOULD be described as open dissipative structures with a dynamic stability sustained by exchange of matter, energy, and information based on a special organized structure–solitons and generation of electromagnetic field.  Microtubules are a cog in this nanomachine.  The organization of atoms in them is the key to really understanding how life operates electromagnetically.









Pokorný J., Jelínek F., Trkal V., Lamprecht I., Hölzel R. Vibrations in microtubules. J. Biol. Phys. 1997;23:171–179. doi: 10.1023/A:1005092601078.


This video blog is designed to show that Thomas Paine and Nayib Bukele have much in common.  

Politically they are doing the same things to their countrymen.

Thomas Paine was born on February 9, 1737, and died on June 8, 1809.  He was an English-born American political activist, philosopher, political theorist, and revolutionary. He authored Common Sense (1776) and The American Crisis (1776–1783), two of the most influential pamphlets at the start of the American Revolution, and helped inspire the Patriots in the 13 colonies of New America in 1775 to declare independence from Great Britain. He wrote Common Sense at the age of 38.  On September 7th, 2021 Nayib Bukele was 38 years old when he made Bitcoin legal tender in El Salvador.  Both of these men were Millenials of their day.  Paine’s ideas reflected the Enlightenment-era ideals of transnational human rights.  Bukele’s political ideas have changed to support the same ideology.  Paine convinced poor farmers who sought refuge from King George over religious freedom and freedom from unjust taxation.  Bukele is doing the same by giving his poor country monetary freedom to fight the lender of last resort known as the IMF.  The IMF represents the same ideology as King George.

What Paine said in “Common Sense” describes Bitcoin perfectly for mankind in 2022.

Paine wrote, “Perhaps the sentiments contained in the following pages, are not yet sufficiently fashionable to procure them general favor; a long habit of not thinking a thing wrong, gives it a superficial appearance of being right and raises at first a formidable outcry in defense of custom. But the tumult soon subsides. Time makes more converts than reason.

As a long and violent abuse of power, is generally the Means of calling the right of it in question (and in matters too which might never have been thought of, had not the Sufferers been aggravated into the inquiry) and as the King of England had undertaken in his own Right, to support the Parliament in what he calls Theirs, and as the good people of this country are grievously oppressed by the combination, they have an undoubted privilege to inquire into the pretensions of both, and equally to reject the usurpation of either.

In the following sheets, the author hath studiously avoided everything which is personal among ourselves. Compliments, as well as censure to individuals, make no part thereof. The wise, and the worthy, need not the triumph of a pamphlet; and those whose sentiments are injudicious, or unfriendly, will cease of themselves unless too many pains are bestowed upon their conversion.

The cause of America is in a great measure the cause of all mankind. Many circumstances hath, and will arise, which are not local, but universal, and through which the principles of all Lovers of Mankind are affected, and in the event of which, their Affections are interested. The laying of a Country desolate with Fire and Sword, declaring War against the natural rights of all Mankind, and extirpating the Defenders thereof from the Face of the Earth, is the Concern of every Man to whom Nature hath given the Power of feeling; of which class, regardless of Party Censures, is the

Philadelphia, Feb. 14, 1776.”

On June 5, 2021, El Salvador President Nayib Bukele declared that bitcoin, the first cryptocurrency, would become legal tender in El Salvador. A few days later, the Bitcoin Law was passed, to take effect on Sept. 7, 2021.

Bitcoin restores and provides monetary freedom to the people.  This is the only freedom that was not spoken about by Thomas Jefferson in the Declaration of Independence of July 4th, 1776.  The reason should be obvious:  the idea of Bitcoin was 233 years away from 1776.  Ironically, the corrupted democratic republic would fund and build the internet that would act like John the Baptist for the introduction of Bitcoin by Satoshi Nakamoto.  Bukele seemed to realize that monetary freedom would be the seed to sow if he wanted to rid his country of poverty and the slavery of IMF debt.  Most of his population however has no idea how this idea works.  Moreover, his political allies want the public to believe that Bitcoin is Bukele’s coin or his idea.  It is far from the truth.

What Bukele gave his people on Sept 7th, 2021 was a new Declaration of Independence from IMF rule. September 7th, 2021 was an action that mimics precisely what Paine wrote above in words.  He gave them a reason to fight for freedom.  Freedom comes in a negative and positive forms.  One is “Don’t Tread On Me” (negative), and the other is “We The People” (positive).   Patriots of the 13 colonies had to fight for their freedom and liberty in a revolutionary war.  The people of El Salvador, today, really have no idea what Bitcoin is or who Paine was and what he did for future Americans, but they do not have to wage war against their King today.  That King is the IMF, their current debt holder.  They just need to buy Bitcoin to fight their King and push him to submission.  People who are forced to use paper money are going to have to fight the peaceful quiet riot until we have to wage the real war against the banking elites.

Bitcoin is more than just a wise investment of the present day.  It’s poised to become the central player in the future of money itself. Money, which has evolved through the millennia from cowrie shells to clay tablets to precious metals, banknotes, and bank balances, is taking another step into the future. Money is becoming digital.  Governments linked to the IMF and BIS want to create centralized digital money called SDRs or CBDCs.   All of these technologies limit the freedom of people using them in a myriad of ways.  This suits the government but it does nothing for the things written in the Declaration of Independence or the US Constitution.

Thomas Jefferson’s words in our Declaration of July 4th, 1776 rhyme quite well with the actions of Nayib Bukele on Sept 7th, 2021.

Jefferson wrote, In Congress, on July 4, 1776,

“The unanimous Declaration of the thirteen united States of America, When in the Course of human events, it becomes necessary for one people to dissolve the political bands which have connected them with another, and to assume among the powers of the earth, the separate and equal station to which the Laws of Nature and of Nature’s God entitle them, a decent respect to the opinions of mankind requires that they should declare the causes which impel them to the separation.

We hold these truths to be self-evident, that all men are created equal, that they are endowed by their Creator with certain unalienable Rights, that among these are Life, Liberty, and the pursuit of Happiness.–That to secure these rights, Governments are instituted among Men, deriving their just powers from the consent of the governed, –That whenever any Form of Government becomes destructive of these ends, it is the Right of the People to alter or to abolish it, and to institute new Government, laying its foundation on such principles and organizing its powers in such form, as to them shall seem most likely to effect their Safety and Happiness. Prudence, indeed, will dictate that Governments long established should not be changed for light and transient causes; and accordingly, all experience hath shewn, that mankind are more disposed to suffer, while evils are sufferable than to right themselves by abolishing the forms to which they are accustomed. But when a long train of abuses and usurpations, pursuing invariably the same Object evinces a design to reduce them under absolute Despotism, it is their right, it is their duty, to throw off such Government, and to provide new Guards for their future security.–Such has been the patient sufferance of these Colonies; and such is now the necessity which constrains them to alter their former Systems of Government. The history of the present King of Great Britain is a history of repeated injuries and usurpations, all having in direct object the establishment of an absolute Tyranny over these States. To prove this, let Facts be submitted to a candid world.”  Jefferson then went on to state the case of facts at that present moment of why freedom from the King’s tyranny was wise for New America.  History has documented this movement 246 years ago.

13 years ago Bitcoin was born.  Bitcoin is the “musket rifle” that Bukele has chosen to use against the IMF for the benefit of his people.

Governments have become quite eager to defend the status quo where states and state-based institutions have a monopoly on money printing, and corporations also have their sights set on the reinvention of money. In this regard, Bukele sticks out like a sore thumb to most other politicians in the world.  He wants to return the freedom of money back to his people for them to decide how to live their life.  But there are a number of factors that over time will work in Bitcoin’s favor.

First, Bitcoin is censorship-resistant and offers freedom from financial repression.

  • Second, Bitcoin is emerging as the natural successor to gold as a store of value over time.
  • Third And somewhat counterintuitively, Bitcoin is benefiting from the efforts of legacy financial technology and payments companies like Western Union, PayPal, Block, and Visa that are making Bitcoin available to their hundreds of millions of users and millions of merchants.
  • Fourth, Bitcoin is being embraced by large public companies and other institutions as a viable alternative to cash and other assets on their balance sheets or in their portfolios.
  • Fifth, Bitcoin’s community is borderline religious in their devotion, which makes Bitcoin resilient in the USA.  This freedom fever is spreading to communities in El Salvador and Central and South America as it did in the 13 colonies during Paine’s lifetime.

Bitcoin is censorship-resistant which creates freedom emergently. In other words, a government cannot throttle, control or monitor your behavior as they can in the legacy financial world. Consider the following examples from Nigeria, Canada, India, Belarus, China, and Russia, collectively home to 3 billion people.

In 2020, protests against the government erupted in Lagos and across Nigeria because of the brutal and illegal actions of a unit in the police force called the Special Anti-Robbery Squad (SARS). Within days, groups supporting the protesters had their bank accounts frozen. With no other option, they turned to Bitcoin, raising funds that sustained the movement.  We saw the same thing in Canada in the winter of 2022 in Canada, when the Truckers began to use Bitcoin to throttle the tyranny of Trudeau.

In Nigeria, daily U.S. dollar peer-to-peer trade consistently clocks in at over $1.5 million USD from a base of zero only a few years ago. Peer-to-peer Bitcoin transactions can be zero-fee, a big break from the much higher fees many in Africa are forced to pay for basic financial services, such as those for remittances which average 9%.  You saw the video above when Salvadorean told us he gave up 30% of his salary to send his money home to Salvador using Western Union.

Nigeria’s young, tech-savvy Bitcoin users are the model for how the global south in Central and South America will soon interact with financial services.  In China, the government wants to replace many transactions with a central bank digital alternative to control the behavior of how people use money to buy things.  In India, the government too high denomination notes out of the circulation to limit counterfeiting.

The demise of cash highlights the need for a digital alternative to ensure private, safe payments between individuals. For example, in China without cash, your access to credit, payments, and savings can simply be switched off if you disagree with the government, a form of financial deplatforming.  We have experienced deplatforming in the US on social media if you have a different opinion from the paradigm in power.  This idea is all around us now and is a detriment to our inalienable rights to freedom.  Bitcoin is a prescription to this illness.

Bitcoin promotes freedom. It enables anyone, anywhere to send, receive or store their wealth. It also prevents governments or corporations from meddling in these transactions. But what type of freedom does Bitcoin provide? Is it a freedom to use or store digital cash or the freedom from an overreaching state?  This shows the world why Bukele is no dictator.  HE is giving his people something tangible they can use to protect them from the government long after he is gone.  This is precisely what the purpose of the founding documents of the USA was about.  Thomas Paine’s pamphlets set the stage for these documents.  Those pamphlet’s changed public opinion in the 13 colonies about freedom and its costs.  I have a sense that Bitcoin’s change to legal tender status in El Salvador will soon do the same for Salvadoreans.  I think we can see this when we look at the megaphone that resides in El Zonte at the Hope House.

13 years ago, the project called “Filling the Love Tank of El Zonte´s Children ” a project created by Jorge Valenzuela and his wife Cristina Guillen by the mentoring of Michael Peterson and his wife Britney Peterson who brought their philosophy of life to Jorge and Cristina.  From this idea came a community that supported a new open-loop community that embraced the use of Bitcoin in a peer-to-peer fashion.  This idea grew so spread monetary freedom to the poorest in El Salvador.  They now go all over El Salvador to show other communities how to use Bitcoin and better themselves and embrace freedom.


Freedom in the republican sense is a social consensus, as the distinction between a master and a slave. Under such a system, interference does not have to be exercised – the master does not have to crack his whip – for it to be present: The mere existence of external, obtrusive forces makes one unfree.

Liberal freedom, on the other hand, is the condition of being free as long as a master does not interfere arbitrarily. ‘Don’t tread on me’, is the cliche that represents this idea.

Bitcoin is based not on the idea of liberal freedom, but on republican freedom.  This is not Bukele’s idea.  Bukele is borrowing this idea from Paine and Jefferson who borrowed it from ancient Rome.  The American Revolution against British domination was a positive conception of freedom = “We The People” in the Constitution of the USA.  It is best described as the ability to dosomething with the aim of realizing a goal or more fully reaching one’s potential.

The positive conception of freedom is a negative concept because it is based on the absence of something, in this case, domination, and a positive one because it relies on active citizenship. For this reason, it offers a more comprehensive approach to freedom, especially with respect to how government and politics operate.

From this wellspring, Bukele borrowed this version of freedom from Paine and Jefferson because it’s this type of freedom that Bitcoin makes space for in El Salvador today because the democratic process facilitates choice. It’s about self-mastery.  This makes Bukele share some traits with Paine and Jefferson.  It also means Bukele respects what happened in ancient Rome.

Bitcoin, as the only decentralized blockchain technology, not only has the advantage of being free from outside interference but also implements various mechanisms agreed upon by its governance protocols to secure that freedom.  This is how Bitcoin creates self-mastery in its code.  Any “interference” to Bitcoin’s protocol has to be deliberated on, and consented to, by the core developers and node operators before it is approved and implemented.  This is very similar to the US Constitution.  For example, amending the U.S. Constitution requires a two-thirds majority vote in both the House of Representatives and the Senate. Then it must be ratified by three-fourths of the legislatures in the 50 states. If the degree of consensus across a wide body of people is a measure of success, then we can see why Bitcoin uses a proof of work consensus to provide for the freedoms of its users.

What Bukele’s political opponents fail to realize is that the Bitcoin blockchain protocol promises both negative freedoms (“Don’t Tread on Me”) and positive freedom (“We the People”) it attracts not only libertarians but also progressives.  This means Bitcoin will eventually attract ideologues in both Arena and FMLN to his Bitcoin policies.  Neither of these two factions of political ideologues realizes that Bukele is stealing their political power right below their noses.

Today, the right and left in the USA do not argue about the truths in the Declaration of Independence or the Constitution.  They both support it.  In the future, Arena and FMLN will come to the same conclusion about Bitcoin.

The US Constitution and Declaration were missing the major part of freedom, namely, the freedom of money.  Bitcoin solves this problem.  El Salvador has solved the toughest problem.  The key is when will the old world political parties realize that Bukele has used the playbook of Thomas Paine and Jefferson to solve the problem that has plagued El Salvador for decades?

It seems his people trust him now, just like the original 13 colonies trusted George Washington not to become a new version of King George under the guidance of our Constitution which provided governance of the newly born USA.  These words are synonymous with the code found in Bitcoin today.


Mankind’s collective ideas on freedom.

Quantum Engineering #8: HOW SMALL IS SMALL?

How small is small?

When we speak about mitochondria which are loaded with electrons and protons we are engaging the physics of the so-called sub atomic world.  We need to understand how size links to thermodynamics.  This is why the physics of elementary particles and their interactions with light are important to a mitochondria.  When things shrink people understanding tends to shrink as well.

Quantum physics confounds people because the “small world” of chloroplast and mitochondria do not act as the world we observe.   The reason behind this, is as the scale of action of the elctromagnetic force changes so does its power.  The electromagnetic force is mush stronger at small scales than it is at larger scales.

To illustrate this point, consider the size of an atomic nucleus is approximately 100,000 times less than the size of a water molecule. Now understand, a water molecule is smaller than the visible light wavelength in a photon by a factor of 1000. So even using our best optical microscopes we couldn’t hope to see or observe a molecule of water, let alone an atomic nucleus. Thus there is an obvious problem of even adequately visualizing the objects in question that life deals with.  It should be no wonder why centralized medicine is blind to what a mitochondriac understands.

When light is in motion, just changing of the electro-magnetic field in space won’t bend light at all. Physics has proved this; a constant electric or magnetic field wont change its behavior at all. The reason is tied to Maxwell’s classical equations on electromagnetic waves. It’s like rising the water level and expecting the waves on the surface to deflect.
But here is where things get interesting for biology: changing the viscosity of the liquid at a certain time interval (day and night) will deflect the wave on the surface. Can a mitochondria change their viscosity by altering the chemistry inside their matrix? Yes, they can.  Now consider hydrogen bonding networks are very dynamic. So dynamic that we cannot perceive how fast they adapt.

The fast adaptive behavior of these H+ networks in water, alone determine the dielectric constant of medium they are within. Normal bulk water has a high dielectric value. Low pH aqueous environments (inflammation) have excessive protons, and has a lowered dielectric value.  Alkaline pH also changes the dielectric constant. The other chemicals in the matrix, like exotic atoms can alter the dielectric values in the mitochondrial matrix. When we alter the dielectric value guess what interaction changes the most?  Viscosity change the most in cells when this happens.  This changes the quality of the semiconductors inside of us and how they work.  It changes how electrons and protons move within our atomic lattice in mitochondria.  This changes how they process energy and information.  The smallest things in you make the largest difference in medicine and health.

Any change in a dielectric value directly alters the electromagnetic force generation capable between things in the water. This changes the viscoeleastic tensions in mitochondria. This changes the size and shape changes of the mitochondria.

This means the adaptive changes of the dielectric constant in the matrix  can directly affect the ability to tunnel protons or electrons well.  When you have this ability to control these things you have the ability to control how biochemistry can work at its basic level. Remember, all enzymatic catalysis is tied to proton tunneling too. The more viscous something is, the more energy needs to be added to get a tunneling effect to overcome the energy barrier. If you can’t overcome this change you lose the ability to quantum tunnel in your mitochondria.

What does non-quantum tunneling look like?

^^^^ Aluminum after a 1/2 oz piece of plastic hit it at 15,000 mph in space.  This is the effect of kinetic energy in space.

In a mitochondria, the electromagnetic force is uber strong due to the small scale.  In this environment, protons are mostly kinetic energy and not mass.  This is why protons tunnel and why they don’t punch holes like those above in the 6 micron membranes in the mitochondria.

^^^^Answer:  You cells were built by nature to select H+ over deuterium in the carbon back bone of things made by metabolism under the direction of photosynthesis.  The sun buries the smallest things in places and your mitochondria has to decipher this treasure map so you can remain healthy and avoid medicine.

To visualize this process think about a wave on a river as a boat passes and the waves interaction with rocks and pebbles on the river’s edge. Those waves can flow around those objects at the water’s edge. Sound waves can go through walls in houses too so you can hear your kid’s rock music while your trying to watch TV. The EMF waves from a cell tower pass through your house to get to your mobile phone or your laptop from a wiFi source. The water or air that carries these waves does not penetrate your walls or the rocks on the river’s edge, but the vibrations in the air or water do transmit those waves to you to feel or sense it.
If you were the rogue element, the hydrogen ion (H+), you would be able to pass through any wall like a ghost with ease. The hydrogen nucleus stripped of its electron in the sun’s core does this routinely. It can expand and spread out to cover the energy barriers in the sun’s core like a ghost, to be close enough to its partner protons on the other side of the wall to fuse together.

Do you understand why small matters now to life?


There is a data paradox in science. Medicine believes they need big data to heal people so they rely on it without ever questioning it, so they created electronic medical records with blue lit screens. Not one person every thought to ask does the medium affect the message when we collect it this way? Those applications have destroyed the patient/doctor user interface and harmed physicians eyes and brains. Their employers have forced this change and the public is paying the pricce of this error.  Today’s PSA: Data matures like wine, applications like fish…….somebody should tell google that 90% of fish are now extinct. I see a similar path for “data science.”

Integrity of scientific data should add to the “signals” in nature; not add to the noise in our lives. In the end we should attempt to always do the right things in wellness even if it’s difficult. Integrity is telling ourself the truth about the data we find. And honesty is telling the truth to other people about the revelations we’ve discovered in our bio-hacks. Today’s environment forces us to stand within a tsunami of EMF, and this typhoon is fully capable of blowing our health away by changing our viscosity.  We can weather this storm because we can learn how to adjust our sails to ride this storm out using the integrity of our questions as our beacon.