NIR light can achieve green light-responsive photolysis with a single-photon process. Be aware that Pharma is attempting to use light to create prescriptions for diseases they helped create. Be aware Big Pharma is getting into the light game to try to improve the effectiveness of bad drugs. You need to understand why they are doing it for diseases like cancer. Many new cases of cancer are linked to SV40 contamination.

@twocitizenships @RobertKennedyJr

2. It is highly likely in the next few years decentralized research will show that 380 nm light action on the mTOR complex changes the chemistry of this regulator to prevent cancer from developing metabolically in a redox shift.

Why?

We now have new data that reveals shifting the mTOR ensemble toward the catalysis-favored state will hinder cancer growth. Light is capable of altering chemical activations via photo catalytic conversions using optical photonics mechanisms.

3. Nematic liquid crystals represent the basic form of compounds. The elongated nematic molecule is optically anisotropic and is characterized by a uniaxial optical index. The birefringence of the molecule is positive, and its optic axis (extraordinary refractive index) is coincident with the molecular long axis.

Below, you can see the spontaneous organization of the structures in a nematic liquid crystal, where birefringence is equal to ne - n0 and is a function of the applied voltage. This is how sunlight self-organizes liquid crystalline matter inside of us to operate.

1. Today's lesson on biophysics. Why does your jizz fluoresce, and why is a black on your hotel sheets a time to learn a lesson? Your gametes are loaded with opsins. Anyone want to guess why?

2. Did you know that neuropsin (OPN5), sensitive to UVA light which releases NO, has been detected in multiple species of vertebrates, including birds, rodents, and humans. This opsin is one of the more common ones in human ejaculation. This opsin is expressed in both neuronal (retina and brain) and epithelial tissues (cornea and skin). Neurectoderm tissues and gamete. Interesting combo huh? What role does it play in human sex?

3. NO regulates sperm capacitation, acrosomal reaction, and sperm motility and may also have an anti-apoptotic effect. Low NO concentrations may physiologically affect fertilization by enhancing the ability to bind to the zona pellucida (ZP) rather than inducing an acrosomal reaction or promoting oocyte penetration. Opsins connect mother to child epigenetically in ways few realize.

1. Today's biophysics lesson: Technology makes you mentally ill when used to excess.

The major non-thermal effect of nnEMF is a net increase of deuterium in the TCA cycle with a change in the pool of hydrogen in the NADPH pool and a loss of melatonin, which causes more deuterium in the cells. This single change destroys cell membranes where DHA is located. DHA controls the lipid cytosocial regions on lipid rafts in cell membranes to perform the movement of electrons on a liquid crystalline semiconductive circuit. The most important one connects the retina to the SCN to control all growth metabolism in animals because it controls the circadian mechanism, which determines how the clock genes work everywhere in your body. When you live in a nnEMF world, say like musicians, you become depressed and quickly collect deuterium in your matrix, and you might kill yourself or become addicted to opiates. We've recently seen it in Prince, the King of Pop, Houston, Winehouse, Cobain, Cornwell, and Bennington. "Non-thermal microwave/lower frequency electromagnetic fields (EMFs) act via voltage-gated calcium channel (VGCC) activation. Calcium channel blockers block EMF effects, and several types of additional evidence confirm this mechanism. Low-intensity microwave EMFs have been proposed to produce neuropsychiatric effects, sometimes called microwave syndrome, and the focus of this review is whether these are indeed well documented and consistent with the known mechanism(s) of action of such EMFs. VGCCs occur in very high densities throughout the nervous system and have near-universal roles in releasing neurotransmitters and neuroendocrine hormones. Soviet and Western literature shows that much of the impact of non-thermal microwave exposures in experimental animals occurs in the brain and peripheral nervous system, such that nervous system histology and function show diverse and substantial changes. These may be generated through roles of VGCC activation, producing excessive neurotransmitter/neuroendocrine release and oxidative/nitrosative stress and other responses. Excessive VGCC activity has been shown from genetic polymorphism studies to have roles in producing neuropsychiatric changes in humans. Two U.S. government reports from the 1970s to 1980s provide evidence of neuropsychiatric effects of non-thermal microwave EMFs based on occupational exposure studies. 18 more recent epidemiological studies provide substantial evidence that microwave EMFs from cell/mobile phone base stations, excessive cell/mobile phone usage, and from wireless smart meters can each produce similar patterns of neuropsychiatric effects, with several of these studies showing clear dose–response relationships. Lesser evidence from 6 additional studies suggests that short wave, radio station, occupational, and digital TV antenna exposures may produce similar neuropsychiatric effects. Among the more commonly reported changes are sleep disturbance/insomnia, headache, depression/depressive symptoms, fatigue/tiredness, dysesthesia, concentration/attention dysfunction, memory changes, dizziness, irritability, loss of appetite/body weight, restlessness/anxiety, nausea, skin burning/tingling/dermographism, and EEG changes.

In summary, then, the mechanism of action of microwave EMFs, the role of the VGCCs in the brain, the impact of non-thermal EMFs on the brain, extensive epidemiological studies performed over the past 50 years, and five criteria testing for causality, all collectively show that various non-thermal microwave EMF exposures produce diverse neuropsychiatric effects. BOOM! If you have a mental disease, you have a bad relationship with the electromagnetic spectrum.

2. All stress leads to this ------>

Lactate--not glucose--is the primary energy substrate in ALL mammals. You should read that again, FOLKS. Now you know that the levels of Vitamin C in the glial cells are linked to the amount of catecholamine made. Is dopamine a catecholamine? YEP. Is dopamine levels related to creativity? YEP. Where is the lactate glucose paper, Uncle Jack? …

Glucose is the monosaccharide utilized by most eukaryotes to generate metabolic energy, and in the majority of eukaryotic systems, glycolysis is the first biochemical pathway where glucose breaks down via a series of enzymatic reactions to produce relatively small amounts of adenosine triphosphate (ATP). In 1940, the sequence of these glycolytic reactions was elucidated, a breakthrough recognized as the first such elucidation of a biochemical pathway in history. Accordingly, the glycolytic breakdown of glucose ends up either with pyruvate as the final product under aerobic conditions or with lactate, to which pyruvate is reduced under anaerobic conditions. Consequently, pyruvate has been designated and is held to be the substrate of the mitochondrial tricarboxylic acid cycle, where it is completely oxidized into CO2 and H2O, while lactate has been defined and being held to as a useless dead-end product, poisonous at times, of which cells must discard off quickly.

More than four decades after the glycolytic pathway has been elucidated, studies of both muscle and brain tissues have suggested that lactate is not necessarily a useless end product of anaerobic glycolysis and may actually play a role in bioenergetics. These studies have shown that muscle and brain tissues can oxidize and utilize lactate as a mitochondrial energy substrate. These results have been met with great skepticism, but a large number of publications over the past quarter of a century have strengthened the idea that lactate does play an essential and, possibly, crucial role in energy metabolism. These findings have shed light on a major drawback of the originally proposed aerobic version of the glycolytic pathway, that is, its inability to regenerate nicotinamide adenine dinucleotide (oxidized form) (NAD+), as opposed to anaerobic glycolysis that features the cyclical ability of the glycolytic lactate dehydrogenase (LDH) system to regenerate NAD+ upon pyruvate reduction to lactate. The free radical signal of cytochrome one is made by superoxide. This free radical is important to keep humming if you want optimal creativity in your neurons.

An examination of scientific investigations on carbohydrate metabolism of brain tissue in the 1920s and 1930s has already revealed that lactate can be readily oxidized. However, due to the prevailing centralized dogma of the carnivore bro science crew, according to which lactate is a waste product, its oxidation was assumed to be a possible mechanism of elimination. This chapter examines old and new research data on glucose glycolysis in muscle and brain tissues. This chapter consolidates the available data in an attempt to form a more accurate and clear description of this universal and very important bioenergetic chain of reactions.

Now, the story is complete, where creativity and chaos are linked.

3. All linked to this redox equation.

Living quantum nanomachines inside our cells can do some unique things. Because cells can sometimes extract the work much more quickly, this gives them more power and range. This is why they favor H+ over deuterium in health and why cancers are associated with altered apoptosis and deuterium build-up.

Decentralized science has written off and set aside many of the centralized answers because they are in conflict with cherished beliefs. The new discoveries are out there, and I am fueled by knowing that I can directly affect my own outcomes. I feel empowered because I can recognize dogma and listen to my intuition and body to guide my choices despite what most mainstream advertising is true.

Centralized science around oncology is just paid-for propaganda. And marketing, at its core, is just legalized lying.

Alternative theories that have been proposed in the last 30 years are like the Whos on the Puff in Seuss's Horton Hears a Who.

We are on the brink of a new age and are about to see a great many people wake up and join in the chorus of change to allow the new discoveries to become mainstream and light shined upon alternative theories.
Science never stands still; only our thinking about it does. Pay attention. Attention is your connection to your vitality and to others because it makes you eager. Eagerness breeds curiosity, and curiosity destroys dogma. When dogma is controlled, the beauty of decentralized science is revealed to show you the right path to travel.

2. Have we had it all wrong about cancer? Mammalian cells need ultraweak -UV light to get past the mitosis phase in the cell cycle from endogenous light. What happens if the cell cannot make this UV light? You get metastatic disease. That flies in the face of centralized propaganda sold in oncology circles.

The normal cell cycle consists of complex pathways that regulate the duplication of all molecules and organelles and their separation into two identical daughter cells. This progresses through four phases: G1 (gap), S (synthesis), G2 (gap), and M (mitosis), and is coordinated by cell-cycle regulators that drive chromosome duplication, chromosome segregation, and cytokinesis. The accuracy of this process is controlled by cyclin-dependent kinases (CDKs) and regulatory cyclins, all powered by UV light biophotons, as well as checkpoint proteins that delay cell cycle progression to detect errors and preserve genomic integrity. More on this topic:

3. Even cancer is a kind of disease of lost geometry due to thermodynamic changes, where cells stop obeying the typical patterning cues of the body in favor of tumorigenesis.

To understand chaos, you must understand how thermodynamics, morphogenesis, and information theory all interconnect. The person who found this link first was Alan Turing.

His 1952 paper on Morphogenesis was the first time anyone began to examine how nature uses math to create a logical information space to build life from abiotic atoms.

How did these ideas become linked, and why did this eventually lead to the creation of the computer and to logic theory based on computation? This juxtaposition might be fun and shocking for you to learn. You have to understand some basics of information theory to make sense of what Turing was doing in his brilliant mind back in 1952.

Biologic researchers are paying much more attention LATELY to mechanisms that "actively erase" and hide memory engrams in the brain of humans to truly understand the role of chaos in building the creative mind.

Why would they do this? If you cannot erase memory, you cannot build a life that is based upon thousands of quantum computers working in unison to skate around the second law of thermodynamics to become the ultimate Maxwell demon.

What do I mean by this?

The erasure of information is what drives entropy to increase over time. Few people really understand this consequence buried at the core of the physics of the organism because it is a consequence of the relation of light to matter in the Universe. It is a consequence of having 1 billion light photons to one atom ratio in the universe.

1. Isn't it funny how there are no carbohydrates pictured in this slide below, huh? You'll hear many so-called "experts," tell you diabetes is a disease caused by sugars and carbohydrates fuels. Some of them are so sure they are correct that they have bet their careers on it. Some of us knew differently 20 years ago.

2. The data always left a crack of doubt in most published studies. The wise know that light travels through all cracks and sunlight is the best disinfectant for nonsense. It turns out that blue light liberates Vitamin A, this turns into an aldehyde and ruins lipid rafts on cell membranes so they cannot respond to electromagnetic signals properly.

3. Moreover, when the Vitamin A is freed it destroys heme photoreceptors in any tissue where melanopsin is. It turns out that every cytochrome protein in mitochondria is a heme-based chromophore photoreceptor protein. Once they are destroyed the mitochondrial engines can no longer work properly = higher heteroplasmy = low redox.

1. TODAY'S LESSON: The Holy Trinity implications of cold should stun you. It creates light inside of cells that is stronger than sun by lowering the wavelength of biophontons created by metabolism. This light powers up POMC inside of mammalian cells.
This information has huge implications. The metabolic trap door exists in our eye, via the leptin melanocortin tract, which feeds the environmental light & temperature data to the SCN.

2. All longevity research currently says that high levels of activity in IGF-1 and mTOR pathways cause premature aging and all the diseases of aging. After I read some new data about mTOR absorption and emission spectra in 2006, I no longer bought that dogma any longer. It helped explain why fit elderly people all had great body composition in my clinic and were not dying but thriving. They all ate a pro-mTOR and IGF-1 diets and many did things to increase both pathways to get better too while in the sun and maintaining darkness at night. This flew in the face of the longevity research published. I knew why the data was contrary to my clinical observations now.

3. No one seemed to realize that mammals had a thermoplastic biochemistry that changes their surface topology with light and their internal topology with temperature variation! These things were never controlled for in any longevity research. Moreover, it was never controlled for in any research on humans or on primates. This implied that mTOR and IGF-1 are required for longevity and not associated with death as centralized conventional wisdom regurgitated! Here is proof I was right and others need to retreat from their diet recommendations.