NEW BLOG OUT: I now believe most modern diseases result from showing a regressive evolutionary path. This is called atavism. In my opinion, most modern diseases manifest by showing evidence of semiconductive proteins undergoing photolithographic engineering inside your tissues to change light frequencies, which alters your tissues' water chemistry. This leads to new and alien bends, charges, and alteration of atoms in your tissues that change the morphology of your body and the physiology of your tissues. The most powerful changes occur in the POMC gene family and all the peptides it creates by light frequency cleavage. Changes in light frequency alter the dielectric potential in water, which sculpts semiconductive design. This is functionally how evolution occurs. It is not the path that Darwin put centralized science on.

My unconventional theory of atavism and photolithographic engineering goes against current mainstream scientific beliefs. However, It is plausible because of the science underpinning the solid-state physics that governs semiconduction and optics. While evolution plays a role in disease development, it is typically understood in centralized science via the lens of genetic mutations and natural selection = Darwinism

The idea of light frequencies altering tissue chemistry and causing changes in the body is not well-supported by current centralized scientific evidence because no one in centralized science is allocating money to study it. BigHarma and the NIH are invested heavily in the belief that alterations of RNA and DNA are how evolution happens exclusively. They do not even allocate 1% of their funding to mtDNA studies. This shows you why decentralized action below the cell level remains hidden from the public. This blog will make you realize just how much they do not know and why we must question their authority on this topic.
patreon.com/posts/quantum-… 2. Proof I am on the right track and everyone is headed off a cliff in centralized medicine. Read this 2017 gem.

I have begun to source out scientists and manufacturers to build me some new devices for my work here in El Salvador. I want a cheaply built handheld high-field EPR spectroscope for me to use in the clinic. I have some new ideas for how to improve public health and break my addiction to MRI scanning.

If you know of anyone who is capable of this send them my way. 2. To understand why I want it, you have to understand the principles behind ESR Spectroscopy. It allows us to evaluate the subatomic world of biology. This is the electronic and vibrational level of tissues to understand the TRUE redox state of the the cell. In centralized science, ESR spectroscopy is a powerful technique used to study the properties of unpaired electrons in paramagnetic species. If you have read my quantum engineering series on Patreon, you will learn about how I hacked the periodic table. This takes the idea to the next level. It provides information about the electronic structure, chemical environment, and dynamics of free radicals, transition metal ions in the EC space and collagen matrix, and biofilms in the body. It also will tell me about other paramagnetic species at a deeper level like oxygen consumption and bio-photon creation.

This is why I embarrass them. I show the audience their ignorance. Just watch Max. I am going to do it now to your heart doc friend.

https://twitter.com/MaxGulhaneMD/status/1784738637529366938

2. Dr. Alo is a straight centralized cardiology idiot. He has no idea about the history of heart disease the clue left for us to discover why what we believe today is ludicrous.

Consider Madame Curie, won two Nobel's for her work radiation and died early because of what she exposed herself too. Most know that story.

What don't 99.9999% of modern cardiologist know?

Marconi discovered the telegraph and stole much of thescience around wireless technology from other scientists who are now lost to history.

Marconi's life and demise is not well known by modern humans. It is a stark reminder of the potential risks and challenges that come with pushing the boundaries of technology and innovation. It serves as a reminder of the importance of taking care of one's health and well-being, even in pursuit of one's passion and goals.

In 1895 Italian inventor Guglielmo Marconi built the equipment and transmitted electrical signals through the air from one end of his house to the other, and then from the house to the garden. These experiments were, in effect, the dawn of practical wireless telegraphy or radio.

Marconi had ten heart attacks after he began working with electricity. the first one happened one year after he began working with the electromagnetic spectrum. Marconi was 63 years old when his tenth and final heart attack killed him. He ate no processed food or seed oils. He did not have blue light but boy did he get a huge dose of nnEMF daily. Do you know that nnEMF raises TG and LDL tremendously? Did you know it raises blood glucose and insulin irrrespective of food?

When the environment changes because a new toxin arrives you have to decipher the message as a decentralized clinician. The first thing you must do is observe the mast cell system in your patients. This sensory system sits between your brain’s immune defenses and the environment. In 1893 our mast cell system underwent systemic unfettered attack because we unleashed a new pathogen into our environment. That pathogen was stray AC electricity.

What did it do?

Mast cells’ job in our body is to coordinate the immune system’s activities that deal with a variety of toxins and infectious agents. When appropriately stimulated by a toxin or infectious agent, the mast cell releases granules, which contain biochemical mediators which are made from aromatic amino acids with variable absorption spectra. Mast cells can make more than 200 biochemical mediators in response to various stimuli. The most common of these mediators are histamine, serotonin, and tryptase. It turns out, nnEMF is a potent stimulus to this system. Chronic abuse of light activates this system while it destroys melanin in us. Mast cell activation is one of the key symptoms I look for in people with melasma or unusual pigmentation changes in the skin due to chronic blue light, RF , and microwave exposure. 2. The mast cell is closely concentrated around capillaries, with large amounts present in the dermis, and is rich in histamine granules, promoting an inflammatory reaction when secreted. The melanocyte, located in the epidermis, produces melanin, a polymerization product of tyrosine. The melanogenesis, therefore, depends on the enzyme tyrosinase, which is stored in the melanosome of the melanocyte. When the melanosome fills with melanin and protein, it turns into a melanin granule, which is phagocytized by keratinocytes. The dendrites of the melanocyte provide an important framework, necessary for the melanocyte to transfer the melanin granule to surrounding keratinocytes. This transfer of information of light directly correlated to skin pigmentation. The number of melanocytes correlated to the mitosis rate postnatal in human. Mitosis can only be allowed to happen in the presence of ultra weak UV biophoton release from cells at night during our dark phase. If this process is disrupted by mast cell activation pigmentation is altered and disease results. Vitiligo is a mast cell activation disease of the skins topology to dirty electricity and stray nnEMF in your environment. Tech abuse increases mast cell activation problems are drives the incidence and prevalence of these conditions

If you think Vitamin C is the antidote to blue light toxicity youre a bigger idiot. Most functional medicine doctors do and they load up IV's to give patients this. This is the fastest way to destroy their patients endogenous melanin sheets in tissues and induces massive redox shifts to cause disease while raising tissue level entropy. I have two patients from famous functional medicine doctors now who developed Marie Antoinette syndrome. Caveat emptor on who packs your parachute. .jamanetwork.com/journals/jamad… 3. A 69-year-old Caucasian man was referred for the sudden and asymptomatic whitening of the hair on the scalp and eyebrows, with a moderate loss of follicular units. The trigger was the death of his brother. Hair whitening appeared 24 hours after the event. The patient denied the use of bleaches or other hair cosmetics. He reported a history of alopecia areata in plaques on the scalp, with spontaneous complete resolution in 2006. His personal history consisted of hypertension, type 2 diabetes mellitus, dyslipidemia, chronic pulmonary obstructive disease, and atherothrombotic occlusion of the left internal carotid artery and chronic use of Vitamin C tablets from his functional medicine provider. The physical examination showed full whitening hair on the scalp and eyebrows. Eyelashes were not affected. The pull test was negative, and the patient denied a significant hair loss in the last days. The histopathological study showed several follicle-sebaceous structures in the anagen, and one of them (inset) with a transforming hair bulb. The anterior bulb was surrounded by a lymphocytic inflammatory infiltrate in an advanced stage of transformation to the catagen and incipient scar changes.
Immunohistochemistry staining showed positive CD8 lymphocytes and anti-PD-L1 antibody expressed in the lymphocytes that infiltrated the hair follicle. Based on the clinical and histological findings, a diagnosis of canities subita in the context of alopecia areata was made. After discussing the prognosis with the patient, an expectant attitude was taken. He decided to vacation in the tropics for the next year given the advice given in the Melanin Renovation Rx. After 12 months of follow-up, a spontaneous repigmentation showing the characteristic pattern in “salt and pepper” was observed, clinically the same as before the episode of canities subita. Immunohistochemistry staining from PD-1 and HMB45 is shown below.

1. What becomes of oxygen we breathe?

Oxygen plays a role in a variety of cellular processes, including sterol and fatty acid synthesis, and is critical for oxidative phosphorylation (8). Thus, it is not surprising that changes in oxygen availability can have drastic effects on the function of a cell. Several studies indicate that low-oxygen conditions can induce apoptosis (76, 86). This occurs when oxygen levels decrease to at, or below, 0.5% (anoxia). When oxygen levels are 0.5–3% (hypoxia), cells do not undergo apoptosis. Instead, hypoxia activates a variety of cellular events that can ultimately lead to cell survival depending on the light associated with the hypoxia signal.

The reduction of oxygen to water by mitochondrial respiration may represent the integration of two essential functions for aerobic life: coupling to oxidative phosphorylation for bioenergetic benefits and elimination of the essential ROS substrate for maintaining genomic stability. This may surprise you.

Low oxygen in mammals triggers signal-transduction pathways involved in both cell death and survival. For example, anoxia activates proapoptotic BCL-2 proteins and caspases to initiate apoptosis.
The adaptive cellular events that occur in response to hypoxia are mediated largely by the transcription factor hypoxia-inducible factor-1 (HIF-1).

HIF-1 induces the expression of multiple antiapoptotic BCL-2 proteins to promote cell survival. Interestingly hypoxia increases production of mitochondrial reactive oxygen species (ROS), which serve as signaling molecules to activate HIF-1. This link shows you ROS is not always a bad situation inside a mitochondria. Inside mitochondria, oxygen role has changed because of how experiments have shown us how redox chemistry is really run. It is now seen to give rise to copious amounts of "diffusible reactive oxygen species" known as DRS/DROS.

Implications? In the field of enzymology, murburn is a term coined by Kelath Manoj that explains the catalytic mechanism of certain redox-active proteins. The term describes the equilibrium among molecules, unbound ions and radicals inside a cell simultaneously. This process signifies a process of "mild unrestricted redox catalysis".
Murburn is abstracted from "mured burning" (connoting a "closed burning", an oxidative process), and implies equilibriums involving diffusible reactive oxygen species (DRS/DROS/ROS) created inside of mitochondria. Though akin to the oxygen assisted combustion of fuel, unlike the flames produced in the open burning process, the biological reaction occurs in enclosed premises, is mild and generates heat alone without flames. The heat is used by water and by melanin. Heat increases melanin's ability to be an electrical conductor in mammals. Exogenous dark skin melanin uses this and endogenous melanin makes use of this in uncoupled haplotypes. Such a reaction can also incur selective and specific electron/moiety transfers quantum mechanically that are not acounted for in biochemistry books.
Further, though burning is a reaction that usually involves oxygen (aerobic process), "burning flames" produced by anoxic oxidants are also well-known. Therefore, the enzymes working via murburn scheme (aerobic or anaerobic) can now be called murzymes and the region around the biomolecule where the DRS interacts with the final ‘substrate’ is called ‘murzone’. Melanin and water are key chemicals allowing murzones to operate. 2. Since oxygen is paramagnetic, what are the effects of oxygen with cell phone use?

Cells phones generate magnetic fields. Paramagnetic atoms are drawn to magnetic fields.

What is the magnetic field strength of a cell phone?
The magnetic field strength transmitted from the antenna of the majority of all cellular phones, about 7.5–10 cm from the antenna, is well over 2000 nT. When a cellular phone is held to the user's head, it emits a magnetic EMFs of 1000 to 6000 nT.

Cell phones not only expose the user to radiofrequency (RF), but also to a magnetic field (MF) of extremely low frequency (ELF: 1 Hz—100 kHz according to the ICNIRP. The ICNIRP tries to minize the physics. So you need to realize all tech use close to your body makes you HYPOXIC.

Statins increases human Coronary Artery Calcium Score and promotes vascular calcification, and the plaque gets harder and the stent becomes more useless but it is great for centralized cardiologists and heart surgeons.

1.

2.

3. https://consultqd.clevelandclinic.o...coronary-atheromas-even-while-shrinking-them/

4.

The use of statins increases the calcific atherosclerosis in T2DM and increases risk of CVD morbidity and mortality - acc.org/latest-in-card…
nature.com/articles/s4151…
tctmd.com/news/statins-.…
care.diabetesjournals.org/content/35/11/… 2. Statins are mitochondrial toxins because of their effect on CoEnzQ10. There are many ways in which they increase coronary artery calcification. One way is depletion of Vitamin K2 from the gut, another is lack of sun to control calcium flows, and another is direct arterial melanopsin damage liberating Vitamin A to cause intimal damage and a loss of arterial NO.

Sufficient production of vital biochemicals such as Geranylgeraniol (GGPP) is required to maintain endotoxin tolerance in macrophages in our arteries once the damage occurs. Macrophages are the hallmarks of CVD/Atherosclerosis, contributing to plaque development, inflammation, and the promotion of thrombosis. Geranylgeraniol is downstream of Mevalonate in the cholesterol synthesis pathway, and GGPP synthesis is inhibited by Statins, as is CoQ10 and K2. Vitamin K2 is the cofactor for matrix Gla-protein activation, which PROTECTS arteries from calcification.

Statin use is independently associated with increased calcification in patients, & using an animal model of hypercholesterolemia, we present a molecular mechanism whereby statins promote the calcification of atherosclerotic plaque. ahajournals.org/doi/10.1161/AT…

The amount of sleep an organism needs is directly tied to how well the organism deals with “entropy dump” back into its environment. If you do not dump it back into the environment well, you need to sleep more. If you dump entropy back into the environment well, you need to sleep less. No one has that understanding of the purpose of sleep because they do not have my understanding of how a quantum cell works. ----said by Moi, 15 years ago in a blog. 2. Each molecule of ATP in a cell controls 8800 water molecules binding sites and 20 potassium ions, to make metabolic water function as a liquid semiconductor inside every cell.  I said this in the podcast 24 hours ago but wrote it in a blog 15 years ago.

A member on my forum recently posed the question, “we hear that ketones are a great brain fuel: they provide more ATP than sugars, burn cleaner, and may possibly be the preferred fuel, etc……….we also hear that ketosis works for refractory seizures and there are case reports and a few small studies showing benefit in autism, Alzheimer’s and possibly other neurodegenerative diseases. It appears most everyone reports sharper cognition and sense of energy/well-being. The confusing part for me is that many people also report poor sleep with ketosis. Why is just changing food, and no other variables, often linked to reports that their sleep worsens? It is a common complaint and I can’t yet make sense of it. Can you explain it to me?

Yes, this explanation came right out of a blog I wrote 15 years ago.  Nobody seems to read anymore.

My Answer using Quantum Cell Theory: The answer to this is easy, yet complex, but buried in the science of the Energy and Epigenetics 6 blog post. When you eat a more ketogenic template you make more ATP to maximally unfold proteins. This is based upon the ability of one mole of glucose only making 36 ATP vs 147 ATP from the beta oxidation of fats. ATP’s main function in a zero entropy quantum cell, opens protein conformational structure to expose more water binding sites in proteins.

When this occurs the amount of ATP is stochastically linked to potassium concentration inside the cell. This is why potassium is found inside all cells and sodium is not. Sodium exclusion is not due to a membrane pump as most biochemistry books say. Gilbert Ling proved this mathematically and experimentally close to 50 years ago. The only reason his work was not accepted was because biology does not realize that energy in cells is generated by semiconduction of charged particles that are separated from water. Becker’s proof on Ling’s conceptual framework did not come until 9 years after Ling showed why K (potassium) and Na (sodium) are included and excluded because of the semiconducting currents found inside cells energized by sunlight. This has been further proven in the molecular actions of rhodopsin, melanopsin work in the retina, and actin and myosin in muscle by Gerald Pollack, all using hydrated protein semiconduction.

1. The discovery of a central gear in the biological clock in 2012 should have silenced the food gurus and biochemists, but it did not because they do not read science that trumps their beliefs.

Two cellular switches found on the nucleus of mammalian cells, known as REV-ERBα and REV-ERBβ, are essential for maintaining normal sleeping and eating cycles and for metabolizing nutrients from food.

REV-ERBα and REV-ERBβ are clock gears in our flow meters for entropy measurement that tell our cells and mitochondria when to sleep and metabolize food. They even explain why drugs like Ozempic and sleeping pills can harm humans.

The findings were reported 14 years ago in the March 29, 2012 journal Nature. In the paper, they describe a powerful link between light and dark cycles that control circadian rhythms and metabolism, suggesting a new avenue for treating disorders of both systems using light and dark alone. The diseases included jet lag, sleep disorders, obesity, and diabetes. Instead, humanity got Ozepmic from BigHarma.

Nuclear receptors in mammals should be targeted with light frequencies and dark times. Instead, the research was used to build drugs like Ozepmic. I laid this case out on the Once Bitten podcast with Daniel Prince. This paper came out right after my banned TED talk. This paper confirmed we should be able to target REV-ERBα and β to treat disorders of sleep and metabolism using light, cold, and darkness. 2. In mammals, the circadian timing system is orchestrated by a central clock in the brain and subsidiary clocks in most other organs. The master clock in the brain is set by light and determines the overall diurnal or nocturnal preference of an animal, including sleep-wake cycles and feeding behavior.

Scientists knew that two genes, BMAL1 and CLOCK, worked together at the core of the clock’s molecular machinery to activate the network of circadian genes. In this way, BMAL1 acts like the accelerator on a car, activating genes to rev up our physiology each morning so that we are alert, hungry, and physically active.

Prior to this work, REV-ERBα and β were thought to play only a minor role in these cycles, possibly working together to slow CLOCK-BMAL1 activity to make minor adjustments to keep the clock running on time.

However, genetic studies of two genes with similar functions can be challenging, and thus, the real importance of REV-ERBα and β remained mysterious to the centralized science world.

Scientists got around this hurdle by developing a mammal model in which both genes could be turned off in the liver at any point by giving them an estrogen derivative called tamoxifen. Those mammals were then allowed to develop normally to adulthood, at which point the scientists could turn off REV-ERBα and REV-ERBβ in their livers —- an organ crucial to maintaining the correct balance of sugar and fat in blood —- to see what effects it had on circadian rhythms and metabolism.

1. A thread outing the nonsense of Peatatarians and a centralized scientist on temperature and Cold thermogenesis.

Why is/was Susanna Søberg, PhD someone to avoid on her ideas around cold?

https://twitter.com/DrJackKruse/status/1658203080276451349

2. Why do you need to be careful with longevity researchers' ideas?

In centralized science, the molecular link between aging and cancer remains unknown. Right now, they are all chirping that DAMPs = damage-associated molecular pattern molecules. Decentralized ideas have buried the centralized ROS/RNS theory of aging by Denham. That idea died too slowly for me.

Aging was widely proposed by centralized advocates to be caused by oxidative injury, wear and tear on the body , cellular senescence, or changes in the neural, endocrine, or immune systems.
Other neo-Darwinist theories consider aging a predetermined process controlled by genes or by the declining role of natural selection.

Of course, to centralized advocates, only some theories currently exist that can explain all of the hallmarks of aging. This idea suggests that aging is a multi-step and multi-event process.

Decentralized perspectives of aging are simple: It is due to a rise of heteroplasmy that lowers the quantum yield of solar light energy transformation, leading to a loss of energy storage at the electronic and vibrational level in the cell. This forces the cell to over-rely on the ancient ATPase system, which cannot fulfill the ATP stoichiometry that human eukaryotic cells require to run their daily programs in a circadian fashion.

Life is always wrapped in opportunity cost to a decentralized thinker. Decentralized perspectives on longevity are both science and art in a unique package blended by perspectives of how the world is affected by Nature. Looking from this vantage point, an excellent decentralized scientist knows they have less time than energy storage capacity, and this pushes him to act, to create, and to share his ideas born in his craft to extend a connection with Nature to pump the system with more solar energy as our biological capacitors fail. Energy collection and storage limit entropy and this gives time its relativity. Time is too precious to waste when you cannot transform sunlight well. Healthy living is maintained by having a vast capacity for energy at any time when it's needed.

DAMPs, sometimes termed alarmins or danger signals, are endogenous molecules released from cells as cells lose ultraweak UV light in response to exogenous and endogenous stressors, especially following injury or cellular death. They play a potential role in the pathogenesis of aging and cancer. DAMPs, however, do not explain aging or longevity to a decentralized thinker.

1. About 100,000 chemical reactions occur in every cell each second. The chemical reaction can only happen if the reacting molecule is excited by a photon."... "We are swimming in an ocean of light, yet few see this light. This light is not present in your biochemistry book or in your theories, is it? Why is this Ray?

The evidence is all around you. Look this picture

Some of us have been resonating this message to the masses for a long time, but you ignore it. Every single molecule you write about, Ray, has an absorption and emission spectrum, yet you have no explanation for why this is the case. ---Kruse to Ray Peat circa 2012 in Washington

It is exciting that the Age of Light has arrived when decentralized medicine is germinating in El Salvador now. The barcode below found in sunlight correlates to the absorption and emission spectra in biomolecules. It controls every aspect of your life, and none of you are really aware of it or its power to help you. My life's goal is to change that about each of you. --- Kruse in 2024. 2. What slides did I show him to try to explain using the old biochemistry text was a bad way to teach influence biological systems that were moving from biochemistry alone to the electronic state of quantum biology that was rapidly advancing.

The Emission of Light by a Hydrogen Atom in an Excited State.

(a) Light is emitted when the electron undergoes a transition from an orbit with a higher value of n (at a higher energy) to an orbit with a lower value of n (at a lower energy).

(b) The Balmer series of emission lines is due to transitions from orbits with n ≥ 3 to orbits with n = 2. The differences in energy between these levels correspond to light in the visible portion of the electromagnetic spectrum. I showed these slide

Both Bitcoin and Nature link together at the level of quantum foam. Why? Bitcoin and mitochondria are time machines that connect directly to the quantum foam by a proof of work mechanism.

A crystal is a solid with atoms or molecules regularly arranged in a particular structure. If one looks at the arrangement with a microscope, one discovers an atom or a molecule always at the same intervals. It is similar to space-time crystals; however, the recurring structure exists not only in space but also in time. The smallest components are constantly in motion until, after a certain period, they arrange again into the original pattern.

The very fabric of space-time at the smallest scales is considered extremely turbulent and chaotic, described as a frothy sea called quantum foam. This concept, stemming from quantum mechanics and general relativity, suggests that the very nature of space-time is bubbling with tiny wormholes and fluctuations that appear and disappear within fractions of a second.

In 2012, the Nobel Prize winner in physics, Frank Wilczek, discovered the symmetry of matter in time. He is considered the discoverer of these so-called time crystals, although as a theorist, he predicted them only hypothetically. Since then, several scientists have searched for materials in which the phenomenon is observed. The fact that space-time crystals actually exist was first confirmed in 2017. However, the structures were only a few nanometers in size and formed only at very cold temperatures below minus 250 degrees Celsius. The fact that the German-Polish scientists have now succeeded in imaging relatively large space-time crystals of a few micrometers in a video at room temperature is therefore considered groundbreaking. But also because they were able to show that their space-time crystal, which consists of magnons, can interact with other magnons that encounter it.

In their experiment, Gruszecki and Träger placed a strip of magnetic material on a microscopic antenna through which they sent a radio-frequency current. This microwave field triggered an oscillating magnetic field, a source of energy that stimulated the magnons in the strip – the quasiparticle of a spin wave. Magnetic waves migrated into the strip from left and right, spontaneously condensing into a recurring pattern in space and time. Unlike trivial standing waves, this pattern was formed before the two converging waves could even meet and interfere. The pattern, which regularly disappears and reappears on its own, must, therefore, be a quantum effect.

@maxkeiser and I are going to unpack this hard science stuff using the art of decentralized networks in our new joint podcast called "Sex at Dawn"

Max brings the artists of decentralization, and I will bring the science. @stacyherbert will be the chef.

2. Did you know MELANIN IS ALSO A TIME CRYSTAL FOR EMBRYOGENESIS IN MAMMALS?

What does melanin do to the quantum foam inside of cells at embryogenesis?

I wrote this blog for @NicoleShanahan to help her daughter. I told her that all the patents Google holds around blue light and NNFEMF have a lot to do with autism.

I wrote this for her daughter: "Embryonic progression in albino mammals’ visual and auditory systems also seems to take a step back in evolutionary time, and it seems this program was initiated by a lack of melanin pigment.  Non-albino animals do not exhibit this altered migratory pattern.  Abnormalities of optic chiasmic misrouting in albino mammals is a developmental field defect that is seen normally in preceding phylogeny. Complete crossing of optic neurons at the chiasm is a normal developmental event in vertebrates before mammals. This reinforces my belief that atavism is a central problem in understanding modern autism."

This was just "one of the punches in the mouth" I gave her that changed her mindset on where chronic disease might arise from the quantum foam of cells. The circadian clock mechanism controls the quantum foam and makes it more ordered and less random.

She decided to fund daylight computer soon thereafter. That computer has no blue light emission. Tell me the quantum foam cannot be used to decentralize medicine. I dare you to. patreon.com/posts/83724567

If you have any skin disease that is associated with an altered immune response, do you know why the sun is your Rx for wellness?

Did you know singlet oxygen is a potent trigger for the induction of human T cell apoptosis.

Did you know UVA light from the sun is the most potent trigger to singlet oxygen production in the skin?

Did you know melanin in the skin augments this effect? I doubt you did because no centralized MD does.

Solar Ultraviolet A irradiation has been effectively used for thousands of years via heliotherapy to treat patients with atopic dermatitis and other T cell-mediated, inflammatory skin diseases.

I BET YOUR DERMATOLOGIST DOES NOT KNOW THE FOLLOWING

In centralized studies of artificial sources of UVA light on the skin of mammals, successful phototherapy of atopic dermatitis was found to result from UVA radiation-induced apoptosis in skin-infiltrating T helper cells, leading to T cell depletion from eczematous skin.

In vitro lab testing of UVA radiation-induced human T helper cell apoptosis revealed that it was mediated through the FAS/FAS-ligand system, which was activated in irradiated T cells as a consequence of singlet oxygen generation.

By the way, clothing and sunscreen block this effect, meaning both cause T cell-mediated skin disease by blocking UV light.


2. Atopic dermatitis is a chronic inflammatory skin disease with an estimated prevalence of 10% in children and 0.5–1% in adults and increasing in incidence by about twofold in 10 yr due to the effects of blue light and nnEMF on the skin.

The pathogenesis of atopic dermatitis is at least in part immunologic and involves a T cell-mediated immune response directed against inhalant allergens and other allergens. Centralized science thinks eczematous skin lesions result from cytokines produced by skin-infiltrating T helper cells present in the dermis.

Decentralized science knows the sun takes care of the wayward cells in your skin that are behind this condition. This is why all these kids have horrendous Vitamin D levels.

Insulin is a solar hormone. Ben does not know that. Sunlight is 43% red light and it lowers blood glucose and insulin. Insulin is a solar hormone and insulin resistance usually is linked to a big lack of solar exposure. Most people with diabetes acquire a dysregulation of intramyocellular fatty acid metabolism because of the lack of proper environmental signaling in the SCN in eye, circadian clocks in the skin which control the clocks in the gut where the beta cells reside. It also turns out that transgenerational diabetes is linked to changes in mitochondrial energy dynamics because of the light mismatch.

Mitchell's membrane pump theory breaks the second law of thermodynamics by 500 fold when we so the stochastic math of the requirement we need to make up how much ATP from food to run the biochemistry of a cell. The energy deficit tells us we cannot make enought versus how much cells need.

This raises a question? How do we do it? Meet melanin and sunlight. Mammals are unique because of how they expanded the use of melanin on our surfaces and endogenously to transform energy from some other place = sun. Water, sunlight, and protons make up the big difference to create the ATP we need. ATP is important but it is not the key to a cell’s bio-energics. Melanin biology is a critical missing piece. Its translation from its GENE only happens when UV light stimulus is present. The UV light generates voltages in our power grid of membranes.

This voltage inside our membranes is what the electromagnetic force of Nature pays deep attention to, as I mentioned to you in Energy and Epigenetics 6 blog. This voltage is directly linked to the cell’s ultimate redox power and redox power is linked to how much light is collected in coherent domains of water in a cell.  

When the voltages are high in membranes anywhere, but especially in the mitochondria, the result is a “relatively stronger current of electrons down the ETC via complex 1. Because the current is strong in one only direction during summer, no reverse electron flow can happen at complex 1, because there is a minimal electron current simultaneously occurring via electron transporting flavoprotein dehydrogenase’s FADH2 at complex 2.

This is where fat electrons stripped from foods enter ECT and where protons are stripped of food. This excess energy from summer time foods is stored as fat when UV light is absent from our environment. This is why carbohydrates can fatten all animals in autumn to ready them for winter. Humans face this too, because they are mammals too.

It is not carbs that fatten us, it is the lack of UV light that is the photoelectric signal that does. This is how we store excess electrons, or highly energized electrons, which are elevated in their energies by the photoelectric effect of the summer light’s power in fat stores. When the electromagnetic force of light is stronger in your environment from non-native solar sources (blue light from tech gadgets) , the results are they we gain more weight because we slow ECT transport. This tells us a problem of the NAD+/NADH redox couple is critical in diabetes and obesity.

We uncouple insulin action from UV light exposure. Non-native EMF causes us to make excessive NADH in our mitochondria causing us to crave carbohydrates. If we eat them when no UV is present, as a result, we lower NAD+, create pseudohypoxia because ECT slows from NAD+ to oxygen. All electrons are delivered to oxygen to reduce it as the terminal electron acceptor. The only reason we breath oxygen is to capture electrons electromagnetically. Not too many people realize this. 2. After the photoelectronic signal for insulin release has been produced in a cell, termination of signaling is also then needed by a cell. How does this happen? Insulin is degraded by endocytosis and degradation of the receptor bound to insulin as a main mechanism to end signaling. Endocytosis needs serious electric forces to be present in the cell membrane for it to happen. So if youre solar deficient, you insulin levels will be higher. This is why nnEMF and blue light are linked to high insulin levels as the picture below shows.

What is the biophysics the food gurus shit the bed on?

It turns out at the center point of insulin molecular structure is an atom of zinc, a transition metal, surrounded by 4 specific amino acid residues with amide linkages. These residues all are quantized to specific light frequencies and are affected by an aqueous surrounding. If those light frequencies are not present insulin never gets degraded properly.

When you ask the ignorant NS who is making money by using radiation with neuralink would not you expect his answer?

Sounds a bit like Upton Sinclair's warning.

The other thing that bothers me about Andrew here is he is supposed to be a scientist who questions consensus opinion. We know Matthew is going to embrace the status quo. Why did not answer bring up the NTP toxicity study which is also non ionizing radiation and ask for an answer on redirect?

For example, Andrew could have said to Matthew, given you answer, "we also know cell phones emit a form of electromagnetic field called radio frequency (RF) radiation. We have long been led to believe that this radiation is harmless because of the low power levels involved, and because it’s non-ionizing." why is it then that the WHO gave perhaps the biggest red flag warning in its history with a classification change on cell phone radiation.

Matthew did you know, in 2011, the WHO finally took a position on the issue and classified cell phone radiation as a possible 2B carcinogen?

I mean you are a neurosurgeon Matthew do you know about the links found with tumors in the organ you are supposed to be an expert in? Cell phone radiation exposure has been principally linked to two types of brain tumors in the PEER literature − gliomas and acoustic neuromas.

Matthew, another Neurossurgeon I have done a podcast with would argue with your opinion. He has relay to his own audience on X that in the October 2006 issue of the World Journal of Surgical Oncology, the investigators reported a 70% increased risk of grade III–IV astrocytomas (highly aggressive brain tumors) for analog cell phone users. This same study found a nearly 4-fold increase in risk for acoustic neuromas after 15 years of exposure to analog cell phones.

Given this data Matthew, should I have my Stanford staff print this study out for you to review so we can re-record your answer now, or should we just ignore this and let Dr. Jack Kruse rip you to shreds on my X feed?



Andrew did not do science. He allowed the guy a pass to continue to propagate bullshit . That is the FACTS.

Now I am more concerned about this behavior than any other behaviors around Dr. Andrew. I don't support hit pieces, but when you have a neurosurgeon who has CONFLICTS due to nnEMF use you better be a fucking scientist and really question him because many people may not know you are help spread propaganda and not promoting hard core science.

Happy Easter to you.ncbi.nlm.nih.gov/pmc/articles/P… 2. Radiation from wireless technology affects the blood, the heart, and the autonomic nervous system, your breasts, ovaries and sperm cells. RF/microwave radiation affects your germline and ruins mitochondrial DNA because it ruins calcium/calmodulin second messenger system of signaling in cells. You do not need nuclear DNA or RNA damage to cause widespread organ dysfunction via the IONIZING part of the spectrum of light. Even RF radiation, on the low energy end of the spectrum of light, causes is as the NTP study just laid out.
Exposure to electrosmog generated by electric, electronic, and wireless technology is accelerating to the point that a portion of the population is experiencing adverse reactions when they are exposed. The symptoms of electrohypersensitivity (EHS), best described as rapid aging syndrome, germline disorders, mitochondrial energy deficits that are more prominently experienced by children than adults and resemble symptoms experienced by radar operators in the 1940s to the 1960s and are well described in the literature and in Robert O. Becker and Dr. Andrew Marino's books. why is that Matthew and Andrew just shit the bed on this science? Might it be it conflicts with their business interests?

An increasingly common response includes clumping (rouleau formation) of the red blood cells, heart palpitations, pain or pressure in the chest accompanied by anxiety, and an upregulation of the sympathetic nervous system coincident with a downregulation of the parasympathetic nervous system typical of the "fight-or-flight" response. The patient becomes chronically dehydrated because of poor water creation due to poor mitochondrial function and blood sugar and blood pressure rises in these cases to varying degrees. Provocation studies have demonstrated that the response to electrosmog is physiologic and not psychosomatic.

Those who experience prolonged and severe chronic electromagnetic exposure may develop physiologic and psychologic problems as a consequence of their inability to work, become fertile, their limited ability to travel in our highly technologic environment, and the social stigma that their symptoms are imagined rather than real. This is what American communication network is doing to the American public's cells and tissues 24/7 now.

5G will ELEVATE THESE RISKS BECAUSE JUMP CONDUCTION IS A FEATURE OF THE ENGINEERING OF THESE WAVEFORMS BETWEEN 6-90 GHz now live in a city near you. The NTP study release of 11/1/2018 was your last official warning. It is time to protect yourself because no one else is going to do it for you. You will soon see unusual human behavior and sickness all around you that shows acute mitochondrial failure from rather innocuous stimuli. The official word on these reports will be lies and obfuscation to control the narrative and maintain control while the profiteers of the internet of things keep harvesting $$$$ from your wallets as you become even more addicted to what is harming you.
Here is my warning: Never underestimate the ability of others to PURPOSELY hide knowledge about disease etiology beneath a carefully curated façade of the illusion of knowledge called settled science. When money is involved character is revealed.

1. Today's lesson comes from a question asked by member Jo. Dr Kruse, "As a BRCA mutation carrier, I was encouraged to do all the prophylactic procedures. Knowing what I know now, I would have never had the double mastectomy hysterectomy and oophorectomy. I now take estradiol, progestin, and testosterone. How can I use the principles of quantum biology to maximize my hormones for the last 40- 50 years of my life?"
2. Answers: The goals are to optimize light, water and magnetism in your environment and maximize your redox power (melanin) because your redox power needs to be uber high to avoid collateral damage in the future. What is redox power? The overall net negative charge left in your cells. Most energy is stored at the vibrational level in cells so your labs and your drug use are not accurate measures of residual redox power. This is the fallacy at the base of functional medicine.

@RobertKennedyJr new running mate, Ms. Shanahan, helped bring this computer to fruition when her ex-husband and his transhumanist friends in Silicon Valley tried to kill it. They want to keep you in their low-dopamine prisons. Ms Shanahan does not want your kids to get autism, unlike her ex, Sergey Brin, who does via his blue light patents he controls 2. When I spoke to Nicole Shanahan the first time, I was not kind to her. I was angry with her. Because of her past, like many of you are now. I had no context. I knew she was a patent attorney married to the guy who holds patents that harm many children via blue light screens. I explained to her that the blue light toxicity was causing transgenerational epigenetic changes in sperm and eggs, leading to many chronic diseases. She told me she never heard of this science. Hence, why I was angry with her. She then told me Brin and her shared a daughter with autism.

I told her I found that interesting and damning. Female children do not get autism easily unless both parents are afflicted with serious blue light toxicity. She was silent as I spoke.

Then, I told her I felt she was complicit in her own child's neurological problem. Centralized medicine believes Autism is a behavioral problem. It is not. It is a migration problem in the developing brain linked to alien light. causing transgenertional epigenetic changes in mtDNA. She was stunned again. It was clear these ideas were new ideas to her. If any of you really know me, you know I am not one to mince words. I was like a drill sergeant to her. I told her it was time to realize what Google was really doing to kids. My own nurse told me I was playing a dangerous game. I did not care. I was hot.

Many people in regenerative medicine want to use exosome technology to extend longevity via drug delivery. I am not interested in this idea at all.

WHY?

Exosomes, called extracellular vesicles (EcVs), are present in almost all cells, tissues, and body fluids. They help in intercellular signaling and maintain tissue homeostasis in disease pathobiology. Researchers have characterized 9,769 proteins, 2,838 miRNAs, 3,408 mRNAs, and 1,116 lipids in exosomal cargo. The separation of exosomes from cells, tissues, and body fluids follows different patterned kinetics. Exosomes interact with recipient cells through their surface receptor.

The transition from interphase to mitosis in the eukaryotic cell cycle is accompanied by dramatic inhibition of endocytosis and exosome action, which leads to profound changes in cellular architecture. Using exosome technology in cells undergoing this transition will lead to massive biological consequences that are not good. If you think this idea is wise, I want nothing to do with what you are up to, much less believe. You'll have to run this race by yourself and live by the consequences of your choices.

A wide range of dynamic membrane functions are inhibited, including protein secretion (Featherstone et al., 1985; Warren et al., 1983), pinocytosis (Berlin et al., 1978; Berlin and Oliver, 1980), and receptor-mediated endocytosis (Warren et al., 1983; Pypaert et al., 1987). Many of the changes in mitosis have been correlated with posttranslational modifications of critical proteins. If I can have any say in the matter, those wishing to employ exosome technology will be on a short leash, and patient outcomes will be scrutinized by the decentralized loop I've designed in El Salvador. @Puncher522 2. Why do cells need UV light to get past mitosis? UV light is required to power up the tubulin proteins that perform the task of cell division or minor ex-vagination inside the cell. During mitosis, tubulin proteins link together to form long microtubules. The microtubules reach from the edges of the cell towards the center to grab and pull sister chromatids to opposite sides of the cell. The application of electric and magnetic fields creates rotational forces on polarized tubulin proteins as the positive and negative sides move back and forth with the changing currents.

Under aberrant forces, tubulin proteins struggle to build microtubules, leading to prolonged mitosis. Impairments in the structural integrity of microtubules can lead to abnormal separation of the sister chromatids, triggering cell death events. This is yet reason two why exosome technology is dangerous to employ without the full knowledge of the mechanism from a quantum biology standpoint. We will be vigilant in protecting the public and informing them of the risks they likely will face.

Today's fun factoid about cancer: metastatic tumors harbor genomic alterations not generally identified in the matched primary tumors. The 2 centralized reasons given in papers for this heterogeneity:

1. Clones harboring these additional alterations are resistant to perioperative chemotherapy.

2. Metastatic lineages arise from early branched evolution in the primary tumors.

DECENTRALIZED REALITY: Its the light dummy

Heterogeneity comes from a lack of ultraweak UV light release, which causes cells to move and mobilize due to a lack of mitosis. When a cell cannot enter mitosis due to a lack of UV light, it stimulates an altered bio photon signature in frequency, stimulating genome reshuffling.

To discover the unknown, we must use the known to guide our thoughts and help us see the future.

If we want to explore the mystery of our mammalian clade, we need to go back to the things that separate us from them and that we know to be true today. The knowns are that our EQ (encephalization quotient) exploded rapidly 2-4 million years ago. WHY? The environment drove changes in our biophoton signature, and this sculpted our RNA/DNA.

New light therapies will be innovated here in El Salvador to highlight these biophysical mechanisms built into cells by Nature that operate against cell cycle machinery components. It will be shown that they can not only repress the division of cancer cells but also reverse cancer metabolism and restore cancer immune surveillance to the mammal. Metastasis will vanish from the human lexicon unless modern gene therapy has polluted their cell machinery by mandate. Few realize that light therapy and heliotherapy provide ongoing effects (4.6 billion years RCT) by transforming light into matter and developing small molecule inhibitors (SMIs) of cell cycle machinery. Modern science shows that PROTACs have recently been used to target oncogenic proteins related to cell cycle progression. This is proof of the concept that Nature is wiser than any lab.

2. Light can reverse mammalian cell division. A protein, PP1, has absorption spectra in the visible light range. The average human body is made up of around 47 trillion cells. Each day, millions of cells die a natural death. So, millions must be divided into two new cells to replace them for life to continue.

While it may sound simple, cell division requires precise timing to avoid catastrophic results, like cancer, where cells divide unchecked, or birth defects caused by an incorrect number of chromosomes.

PP1 tells mammalian cells it’s the right time to divide.

Before cells divide, the chromosomes make copies of themselves. When it comes time to divide, they line up like two rows of runners facing in opposite directions. When enough PP1 is concentrated on the chromosomes, it tells us the cells are sampling a ton of UV light stimulus to facilitate cell division. It also gives the start signal for the chromosomes to separate and race toward opposite poles of the cell along the mitotic spindles.

In 2000, the healthy life expectancy of Americans ranked 38th in the world.

In 2019, we were 68th – behind China, Cuba and Jamaica

Yet, we spend $1.5 trillion more per year on our healthcare system than other wealthy countries.

Americans' ROI is horrendous due to the PEER review process and how big Pharma controls the Journals and the editors.

Big Pharma funds most clinical trials and, therefore, controls the research agenda, withholds the actual data from those trials as corporate secrets, and shapes most of the information relied upon by health care professionals.

In El Salvador, @ZorpZK and I will seek to end that power by decentralizing the Oracle problem that sits in the process. 2. PEER review is supposed to validate methods and data so to predict that a trial is reproducible many times over so we can accept it as truth. It turns out 70% of centralized PEER review is not reproducible.

Consider another pivotal question: Do peer-reviewed journals perform for the public good?

Peer review axioms: Your peers get to review the data.

Except that they never do.

One of Big Pharma’s best-kept secrets is that the peer reviewers charged with ensuring the accuracy and completeness of clinical trial reports published in medical journals do not even have access to complete data and must rely on corporate-influenced summaries. This is often the same for the experts who write the clinical practice guidelines that define our standards of care. This means all evidence-based protocols are opinions of those who pay for the opinion.

Today's lesson: hypothyroidism as a co-morbid condition increases melanoma incidence and prevalence and more importantly promotes melanoma spread. Why? Lack of AM sunlight is the answer. AM sunlight is used to create these hormones and facilitate their release in the HPA. So when you cannot generate enough it menas you cannot generate enough of anything distal to it in this pathway. As a consequence endogenous melanin and dopamine are broken down during tissue hypoxia and a lack of sun. See the topline of the slide below. Few people realize that T3 and T4 are made from the same aromatic amino acids as melanin. Your experts need to read more in dermatology. The sun prevents hypothyroidism, Parkinson's disease, and melanoma. Lack of sun creates the conditions of existence to allow these diseases to manifest. ncbi.nlm.nih.gov/pmc/articles/P… 2. NEW BLOG ON THE BIOPHYSICAL ORIGINS OF DIABETES AND HYPOTHYROIDISM

Almost 80% of T3 at the paraventricular nucleus originates from the peripheral conversion of T4 in cells outside the brain. Only 20% of hypothalamic T3 crosses the blood–brain barrier directly from the periphery. This makes T3 much more important in the human brain. Melanin and DOPA can be used to stimulate T3 production in the brain even when the thyroid is defective or missing.

The more one can tan the better this ability is. Most hypothyroid/diabetic patients are horrible at tanning because their skin is atrophic due to a lack of alpha, beta, and gamma MSH. Regular exposure to solar UV light via your eyes and skin stimulates your thyroid and brain to make T3, which balances your body's metabolism. Tanning increases your metabolism, which in turn helps you maintain a healthier weight. This is all done via POMC biophysics. Anything that blocks it fattens you and ruins your thyroid function.

T3 is the biophysical manna of longevity for mammals. T3 function is the best predictor of longevity for the human myocardium and CNS/PNS. These are the two tissues that kill humans the most. You won't hear that from Peter Attia in his new book on longevity. This completes the lessons I gave you about thyroid function in the cold thermogenesis series of blogs.
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