☣️ Pleb Kruse = BTC foundationalist in exile 🟩🔆 Profile picture
I am a neurosurgeon on a mission to create health from disease by decentralized thinking & BTC! Bitcoin pleb decade club in exile https://t.co/W4I1WtqhJY
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Apr 20 6 tweets 4 min read
Since today is resurrection day what would tell a guy standing outside a cave with healed wounds? I know must of you would say get some sun. But I am thinking about his future longevity?

I would tell them the truth about the biggest scam in the longevity world. Everyone knows that exercise is good. Do you know that exercise has a dose-response curve?

Did you know weight lifting is beneficial in lowering all-cause of mortality in CVD and cancer until you hit approximately 140 minutes a week...So exercise/weight training has a context. Did your doctor tell you this?

More than 140 minutes a week, then your risk of death actually increases. So if you do not want to revisit the cave and the shrouds you had on you might want to take a look at those slides because the food guru biochemists won't tell you this. Their knowledge is all from the DoD, DoE and DARPA.

Do you believe the phrase, "Praise be to Orwell because he gave humanity the antidote to the mind poison of tyranny."

Big Harma money produces the centralized science it wants. Yes or no?

The hallmark feature of Deep State scientific programs linked to DoD and DARPA is to refuse to cite anything that runs against their agendas. The whole truth and nothing but the fucking truth even it offends your ancestors. That is what we tell guys who just came back from death.Image 2. My second thing to tell him.......avoid creatine by opting for your Daddy's light every AM. Key part of staying out of the cave. Mammals who see sunrise always default to a TCA cycle that spins with the clock........those who break the rule go spinning counter to the clock and they are always running around looking to buy creatine from GNCs. Do not be them.Image
Apr 19 16 tweets 10 min read
yes I can. 1. To address how a dose of LSD, known for its effects on absorption and emission spectra and the release of massive ultraweak photon emission (UPE), impacts myelin, we need to consider the biophysics of LSD’s interaction with neural tissues, the role of myelin in neuronal function, and the potential effects of UPE on cellular structures. This response will integrate insights from neurobiology, biophysics, and photobiology, while aligning with the photo-bioelectronic framework of my decentralized medicine thesis. So if you have not read my work or the book below, you'll be shit out of luck. But I have the goods. Given the complexity of LSD’s effects and the link of UPE’s impact on myelin biology decentralized medicine can explain this picture of LSD retinal toxicity.Image
Apr 19 9 tweets 9 min read
Why will prion disease disease be a collateral effect if you do not develop the turbocancer first? @Kevin_McKernan

TIME TO LEARN SOME BIOPHYSICS FOLKS BECAUSE YOUR BIOCHEMISTRY EXPERTS ARE IGNORANT.

Throughout 4.5 billion years of molecular evolution, proteins have evolved in order to maintain the spatial proximity between aromatic residues (Trp, Tyr and Phe) and disulfide bridges (SS) (Petersen et al, 1999).

There is a very special spatial geometric relationship that exists because the process is quantized to light frequencies that our star releases to us on Earth wirelessly. This has not been well appreciated by modern healthcare. This is also why the sun reduces all-cause mortality and why it can never be replaced in healthcare. To suggest this is lunacy when you understand biophysics well.

The interaction of the most powerful part of the solar spectrum of light (UVA/B/C) measures the collisions in the aromatic amino acids and in the disulfide bridges. The aromatic amino acids location becomes the first step in determining where the position and geometry of residues to act as nanosized antennas in the protein world that can capture UV light (from ~250-298nm). Think about my Vermont 2018 video now in this light!!!

The first two protein bends are always determined by nuclear DNA coding. The last two bends are tied to the redox state which is linked to this quantum photoelectric process I am describing here now. If the folding is off you make glitches in folding or bubbles in Muller cells.

Once excited by the incident ELF-UV light these amino acids can enter photo bioelectric signaling that ultimately controls the biochemical pathways likely to have harmful or beneficial effects on protein structures by affecting specific bonds like disulfide bonds in cysteine/cystine.

These two amino acids are the rarest amino acids in our proteins, and as such can acts as the ideal photo-optical switch or gate for signaling because of they a relatively rare in humans.

It turns out cysteine/cystine disulfide bridges in proteins are known to be excellent quenchers of the excited state of aromatic residues by UV light in the literature. This means these disulfide residues naturally decrease the power present in UV light created in the nearby excited aromatic amino acids of the skin.

In this way, they contribute to protein stability and activity in the skin, thereby, stabilizing ubiquitin rates and lowering cancer risk. UV light excitation of the aromatic residues is known to trigger electron ejection from their side chains (Bent & Hayon, 1975a; Bent & Hayon, 1975b; Bent & Hayon, 1975c; Creed, 1984a; Creed, 1984b; Kerwin & Rammele, 2007, Neves-Petersen et al., 2009a).

These electrons can be captured by disulfide bridges in things like glutathione, leading to the formation of a transient disulfide electron adduct radicals, which will dissociate photoelectrically, leading to the formation of free thiol groups in the protein. what you did not know until my Patreon blogs in the last decade is that DDW water from the matrix recycles endogenous glutathione. When it is broken CCO is broken and that means so is apoptosis so mtDNA cannot get rid of misfolded proteins. This is why prions are spiking in a post COVID world.

This photo bioelectrical lever controls the biochemical change then leads to non-optical signaling at deeper levels in the skin. Once disulfide bonds are broken in this way, we can inactive detrimental cell membrane receptors that cause epidermal cancers like EDGF and Herceptin.

The irony in all these detail is that UV frequencies prevent, and do not cause cancer, by these mechanisms.

More irony for the skin, eye docs, and idiot food guru biochemists: This mechanism is now being used by big-pharma to develop drugs using nanotechnology and the ability of cells to make ELF-UV light in a process called LUMI.

When you know better you become a SAVAGE. Never forget it.Image 2. Question asked of me yesterday on my forum. Image
Apr 16 9 tweets 3 min read
1. I know what the collateral effects are.

Cholesterol LDL will rise tremendously in those who sense the change. Cholesterol has minimal absorption in the visible range (>400 nm), making it less responsive to visible light stress but potentially more sensitive to UV light. 2. Other Health Consequences that should be present?
Increased Risk of Childhood Leukemia: Some epidemiological studies suggest a possible link between prolonged exposure to ELF magnetic fields from power lines and a small increase in childhood leukemia risk, though causality remains unproven. Marino’s concern about energy flows suggests this risk may be underestimated due to suppressed research.
Apr 16 11 tweets 7 min read
My photo-bioelectric take is similar to yours on myelin, where we differ is the evolution of myelin.it became a big story 425 million years ago with fishes with jaws. These are the same fish where opsin expansion was done. This is why the modern human brain is filled with melanopsin, encephalopsin, and neuropsin. This means myelin biology and its evolution are linked to a powerful light story. I shared that light story with Nick Jikomes in his pod.

The default state of life was sleep and we evolved wakefulness. Myelin biology occurs post Cambrian explosion by about 200 million years after our G class star starts kicking out more UV light. Physics says it was between 10-20% for our star. So it took life about 200 million years to make use of that light to help sleep. As more Ultraweak biophotons could be created between mtDNA, heme proteins, and melanin this fueled the evolution of myelin so that we could reduce our need for sleep so that we could become more complex. Encephalization in mammals really stresses this situation. Myelin has two major purposes. One is optimizing membrane function for sure in CNS and PNS. No one should deny this, but the other issue that is very murky for centralized biology and biophysics is how white matter links to UV light and oxygen use. Myelin innovation in my view comes out of the GOE. The GOE begins as an oxygen holocaust but then the later spike of UV that happens changes the biophysical mix. 2. @trikomes and I did not talk about this in my pod with him but Why Myelin Evolved in Response to UV Light
1. Evolutionary Pressure from UV Light Post-Cambrian Explosion:
The Cambrian explosion marked a period of rapid diversification of life, driven in part by increased oxygen levels and UV radiation. I’ve noted that 200 million years later (around 338 million years ago), a UV surge occurred as our G-class star increased its UV output by 10–20%. This aligns with the Devonian period, a time when jawed fishes (the first vertebrates with myelin) emerged, around 425 million years ago.

Myelin’s evolution in jawed fishes coincided with opsin expansion (melanopsin, encephalopsin, neuropsin), as you’ve pointed out. Opsins are photoreceptor proteins that absorb UV and visible light, suggesting that light played a pivotal role in the evolution of the nervous system. This should not surprise anyone because MS has a UV light link via its latitide etiology. Myelin, as a lipid-rich structure, evolved to optimize bioelectric signaling in this light-rich environment, supporting the rapid nerve conduction needed for more complex behaviors in vertebrates.

From first principles, increased UV light would have amplified ultraweak biophoton production in cells, particularly from mtDNA, heme proteins, and melanin (as I’ve described in my thesis I shared with Nick).

Biophotons, emitted in the 400–700 nm range, are a byproduct of oxidative processes in mtDNA and can influence cellular signaling. Myelin, with its high lipid content, had to have evolved to harness these biophotons, either by absorbing UV light directly (200–350 nm, as inferred in my thesis) The other possibility is that it could have occurred by interacting with biophotons emitted by nearby melanin or heme proteins in RBCs. This photo-bioelectric role would have reduced the need for prolonged sleep by enhancing energy efficiency in the nervous system, allowing for greater wakefulness and further encephalization.Image
Apr 7 6 tweets 10 min read
This is the entire decentralized thesis that I came up with after spending in 18 months in the medical school library putting Nature's recipes altogether 20 years ago. It lays out in detail what I shared with Nick Jikomes in our podcast. patreon.com/posts/decentra…

Nature is a clever medicine........

Under the wild canopy of Nature, where the river roars and the earth pulses with untamed life, I faced my weakness, a jagged, gnawing disease that clawed at my bones and spirit, threatening to bury me alive. But you, my friend, stared into my soul with eyes like wildfire, demanding forgiveness in a voice that shook the leaves, and together we forged a pact, a sacred vow to banish that cursed word, a sickness, into the abyss, never to haunt us again. Out here, amidst the tangled roots and relentless winds, we dig at each other’s truths, unearthing the raw, beating heart beneath our scars; when my ego flares like a storm, you summon the me of yesterday, strong, unbroken, yet refusing to let me drown in shadows.

Sing it loud, let the branches quake with our anthem, a defiant cry that we’ll always have each other when the world crumbles to ash! Nature’s fierce breath, like moss on my skin, sun igniting my veins, and tears apart the chains of what once held me, reversing the unfairest of fates, while you dig me up from the wreckage, fanning the embers of my better self. Everything else may burn away, but here, under the leaves, our bond is a wildfire, unstoppable, eternal, alive.

She is clever because she is fully decentralized....... 2. The next big question in DMs and emails I received from this pod with PhD @dralexisjazmyn was how we deleted Vitamin C genes and how this was related to UV light and hair loss.

ANSWER: How do you get past the nuclear membrane once you electromagnetically make Vitamin D in the skin? Sunlight energy is also used to sulfate cholesterol FIRST to get the Vitamin D train rolling in the skin to the blood to get to nDNA. When it is sulfated, it becomes water soluble in blood. When it isn't sulfated, your liver responds to protect the nucleus in cells, and it upregulates LDL production to act like a sponge to protect the AMO physics inside of cells. So, when your centralized dermatologist tells you to stay out of the sun and take the secosteroid Vitamin D from a plant or animal, it is also packaged in seed oil because it is normally a fat-soluble compound.

Few realize that the simple act of taking D3 pills and living indoors behind glass walls is raising your LDL cholesterol constantly. BigHarma knew it, which is why BigHarma taught every doctor since they found the evidence in the 1950s military documents that they could profit massively by training doctors ignorant of light's effects to put their patients on statins. They knew to blame it on biochemistry gone awry and baited the PhDs with the papers on the mevalonate pathway Q cycle.

The mevalonate pathway is a sequence of cellular reactions leading to farnesyl pyrophosphate, the common substrate for the synthesis of cholesterol, dolichol, dolichyl phosphate, and CoQ10, and for protein prenylation (a post-translational modification necessary for the targeting and function of many proteins). When you review the history of the evidence, you know they are playing you like a fiddle. You are their mouse, and they are the cat. Few see the game plan, and even fewer of you get it. Cholesterol and Vitamin D3 are nearly identical in chemical structure. Most people need to learn this. Sunlight naturally sulfates these things. The only difference in both bio-molecules is a single double bond in the second ring of the cholesterol backbone. Remember, light is BURIED at the electronic level in all things, including cholesterol and Vitamin D. Your pills are sold to you soaked in seed oils because it is a fat-soluble vitamin. But do we transport it as such? NOPE.

The act of seed oil addition is done on purpose by design because BigHarma knows what deuterium vs hydrogen can do. They've known about the effects of deuterium in drug delivery because of the physical chemistry trials they have done. They never disclosed this to their curriculums to medical students or pharmacy students by design.

This is why they want centralized pharmacies like WalMart, CVS, and Walgreens versus compounding pharmacies. When the drugs are ready-made, all one needs to do is count the atrophy of one's chemistry skills. A compounding pharmacist is an alchemist of physical chemistry. They are more apt to realize what Pfizer and Moderna are up to in New Jersey factories. The AMO physics of these two biomolecules are nearly identical, with one exception. HYDROGEN. This gives Vitamin D3 one less hydrogen atom than the closed ring of cholesterol has. Suppose you have spent any time reading my Tensegrity 6 blog about the original hacks of the periodic table I did 20 years ago. In that case, it should make you think a lot more carefully about atomic details. One hydrogen is the only difference at the atomic scale between them, but from the quantum thermodynamic perspective, you learn that there is a shit ton of energy buried in hydrogen's bond at the electronic and vibrational level. These are the bonds that food gurus and biochemists do not see, much less understand, so they ignore it at your peril. Here is why public health goes awry: because of a lack of focus on what really matters in a cell. Here, you will see the wisdom of my lessons in the Tensegrity 6 blog at play. Look at it all: the charge density sunlight adds to the system that a pill cannot. See, never divorce biophysics from biochemistry. If you do, you lose. The photonic energy in sunlight is used to oxidize hydrogen sulfide to make sulfate. This process sulfates everything at our surfaces and just below the surface, and this makes many things water soluble and lowers charge density. Sunscreen was innovated by BigHarma to block sulfation by design. When you block sulfation, you create a need for more drugs because you lower the tissues in energy, and this exacerbates the timing mismatch in mtDNA. This fuels more mitochondrial mutations and creates disease phenotypes, which fuels their centralized business models. A cursory review of what sulfation does to photovoltaics tells you how Nature uses sulfation to get past a highly charged membrane.

Sulfation from solar exposure makes the fat-soluble vitamin WATER soluble to travel in the blood with VDB. It discharges the charge density to ruin the capacitance of Vitamin D. This is how you enter the nDNA environment like a ghost using the physical chemistry and photochemistry of the nonvisual photoreceptor system in your skin. Nature uses more magic than sunlight. Melanin, Vitamin D, cholesterol, heparin, and nitric oxide all respond to the UV part of the spectrum when it is in sunlight. Few people know that the UV and blue-green parts of the spectrum work in unison to very locally vasodilate blood vessels in the skin. I showed people the melanopsin 2014 paper 1000 times, which showed that blue light is capable of dilating blood vessels, but not one person asked me about the AMO physics of the interaction. This area interested me as a neurosurgeon because I was looking for a mechanism to explain the queer things that happen in brain bleeds called subarachnoid hemorrhages. We see them in trauma and in aneurysm ruptures. I have always felt that a lack of light operating in unison is behind most of the cerebrovascular pathologies that neurosurgeons treat. It took me ten years to figure it out, but altered light signaling is why AVMs and aneurysms rupture. It is also why some people develop SAH with minor trauma. They are all symptoms of low redox power in the brain. Nitric oxide (NO) is a well-known “gasotransmitter” in the literature because a Nobel Prize was given for its discovery in 1992. It is a gas that acts focally and locally when it is released. It does not have global effects. This tells you something about TIMING, too. It acts RAPIDLY, not CHRONICALLY. Vitamin D acts CHRONICALLY. This tells you that NO signaling is likely behind many light-induced chronic diseases. Electrified membranes absorb gas and turn it into many other biomolecules. Life figured this out 3.8 billion years ago. NO is a gaseous signaling molecule that has a unique ability to induce a relaxation of the artery wall and a resulting drop in blood pressure. Recall from my "Kruse for Dummies" lecture what I said about unique signals. They are how information is transferred in biological systems by Claude Shannon's theory of information. Everyone else is playing checkers, looking at biochemical pathways, while I am playing 4D chess because I understand how light operates in physical chemistry. Without full spectrum sunlight, endothelial dysfunction and peripheral arterial damage should be EXPECTED by the decentralized clinician. It is not. No one in medical curriculums looks at the data in BigHarma literature to see this data and much less understand the clinical significance. A lack of NO production at our integument and eye surfaces ALWAYS links PAD by way of intimal thickening = directly to cardiovascular dysfunction. The local effect becomes generalized in the entire organ as the lack of NO production gets worse under ALAN or nnEMF influence. This is why PAD is always linked to cardiovascular disease. The link is the aberrant use of the electromagnetic spectrum to communicate and create NO. Modern light RF and cell radiation impair the production of NO from arginine by eNOS. This, in turn, induces high blood pressure by causing endothelial dysfunction. Mitochondria are intimately involved in importing nitrogen into tissues to create the substrates that eventually become NO when sunlight is present. Nitrogen substrates are not created by direct eNOS synthesis. Nature provided a clue to me as to why humans got rid of Vitamin C genetically for glutathione in this AMO physics dance. When Vitamin C is missing in subcutaneous tissues, glutathione becomes more reactive with locally produced NO. This mimics a radical pair or triad effect we see in avian compass navigation. Here is more evidence of magnetochemistry in humans being used. When glutathione and nitric oxide are powered by terrestrial sunlight, this allows humans to produce S-nitroso glutathione (GSNO). I think this is why human primates lost the majority of their integumentary hair and absorbed more melanin from the hair follicle to the interior. This allowed the skin to become a better charge capacitor for the brain and heart by allowing the skin to become a depot station to store massive amounts of nitric oxide. This is why human immune T cells are so common in the skin and why leptin was placed in SQ fat. Other primates do not have these phenotypes even though their genomes are close to identical. This tells me that magnetochemistry timing (NO is a magnetochemical due to its one unpaired electron) induced this evolutionary change. We never need genes to change this. DECENTRALIZED MEDICINE 101 is why we lost our hair and why we no longer have Vitamin C genes. youtube.com/watch?v=DBF5Cl…
Apr 5 18 tweets 15 min read
New podcast with Nick Jikomes on the evolution of man from oxygen and light selection. A quantum evolution. A new story of paramagnetism that led mammals to a photo-bioelectric method of regeneration and repair.

The lesson is simple: One should take no idea for granted. We should challenge everyone, god, evolution, loved ones, colleagues, supervisors with deep and meaningful questions to the mysteries in life.

We tease out why that is needed today for MAHA.

x.com/trikomes/statu… 2. If you put a pulse ox on the finger below like I do when my patient has Raynauds you can teach youself something about paramagnetism and metHb and NO biology linked to blue light exposure. Blue light changes the oxidation state of Hbo2. Cold immersion brings it on because of the spectra of mtDNA in this patients too: They are all Warburg shifted. This is why they all have higher BG, insulin levels and Hba1c. LIGHT controls this.

Reynaud Syndrome = you have too much time in light that causes iron to be in the +3 oxidation state and this changes the photo-biolectrics of the lipid membranes. You get the cold response of whie skin due to focal hypoxic. I told everyone about the paramagnetic toggle switch in Vermont in 2018. Not one person ask the question since that slide was made. Bottom left of the last slide. Nick and I laid out the whole story in the pod above.Image
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Apr 3 8 tweets 5 min read
1. Such a bad idea. 2. Where is he gonna put the sensors? Skin right? If he does this, what is likely to happen? My decentralized predictions? Image
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Mar 31 10 tweets 9 min read
Check out my latest article: THE SILENCE IS US: Unlocking the Decentralization to Hear the Cosmos

linkedin.com/pulse/silence-…

In 2025, humanity stands at a crossroads, grappling with impossible questions, like monetary collapse, cosmic isolation, and the limits of our own minds that demand more than logic alone can offer. Embracing the suck of the problem can expose the raw, messy struggle of failure and uncertainty. By doing so it unleashes our divine gift of creativity, a force that thrives in chaos and forges unexpected bridges between despair and revelation. It’s through this gritty, unpolished process that we tap into the sacred spark within, transforming the unbearable into the extraordinary and finding answers where none seemed possible. 2. The path to meaningful change, as echoed in my words, demands resilience, action, and unwavering belief in your mission: "Never stop just because you feel defeated. The journey to the other side is attainable only after great suffering and you realizing you have to change your game plan when it FAILS you." For a clinician or a scientist becoming a champion for humanity’s bioelectric health, this means that ideation without execution leads to the deletion of even the best ideas. These concepts of mitigating nnEMF or blue light exposure remain useless without real action that moves the needle. As I've said countless times, "If you go ALL in I will not let you fall. I will catch you, drag you to the finish line," emphasizing that true progress comes from adapting on the fly, because "sometimes not getting what you want is a wonderful stroke of luck."Image
Mar 30 5 tweets 5 min read
Once Massie gets the Senate seat in KY we need to push for a Marshall Plan for Palestine after we get rid of dual passport politicians who are putting Israel's needs before the USA. @saifedean

We need to know some science to pay for this rebuild, but I do know a way I would get it done. It is a story about the minerals beneath the Dead Sea? The value of the minerals and chemicals in the Dead Sea is estimated in trillions of dollars.

Volume of Reserves: The Dead Sea contains an estimated 43 billion tons of salt alone, alongside vast quantities of magnesium, potassium, and bromine. These reserves are replenished naturally to some extent by inflows from the Jordan River and underground springs, though extraction exceeds natural replenishment today.

Industrial Demand: Potassium chloride is critical for global agriculture, bromine has wide industrial applications, and magnesium is increasingly valuable in manufacturing (e.g., lightweight alloys for vehicles). The global market for these minerals supports their high valuation.

Extraction Infrastructure: Companies like Israel Chemicals Ltd. (ICL) and Jordan’s Arab Potash Company have been extracting these minerals for decades, generating billions in revenue annually but not returning that value to the people. Scaling this up over the long term, combined with untapped reserves, contributes to the trillion-dollar estimates.

So the money to rebuild what they have destroyed is there. And if you think about the IDF might have done them a favor to give them a new home to inhabitf for the next 3-5K years.

The Dead Sea’s mineral wealth is the result of unique physical and geological processes rather than evolutionary ones (since "evolutionary" typically pertains to biological development, and no such mechanism directly applies here).

Key factors include:
Endorheic Basin: The Dead Sea is a closed, or endorheic, basin with no outlet. Water flows in primarily from the Jordan River but cannot flow out, leading to accumulation of minerals as water evaporates. This has been ongoing for millions of years, concentrating salts and other compounds.

Low Elevation: At approximately 430 meters (1,410 feet) below sea level, the Dead Sea is the lowest point on Earth’s land surface. This extreme depth enhances evaporation rates due to high temperatures and aridity, leaving behind dense mineral deposits.

Tectonic Activity: The Dead Sea lies within the Dead Sea Rift, part of the larger Great Rift Valley system. This tectonic depression formed about 3-4 million years ago, creating a basin that trapped water and minerals. Geological uplift and faulting also brought mineral-rich brines from deep underground to the surface, adding to the lake’s composition.

Evaporation Over Time: With an evaporation rate exceeding inflow (especially as human water use has reduced the Jordan River’s contribution), the Dead Sea has become progressively saltier. Over millennia, this process has precipitated minerals into thick layers beneath the surface, some of which remain untapped.

Unique Chemistry: The interaction of freshwater inflows with saline groundwater and volcanic activity in the region has enriched the Dead Sea with a diverse mineral profile. For example, bromine concentrations are unusually high due to ancient marine incursions and subsequent concentration.

Why is it worth Trillions?
The trillion-dollar valuation arises from the sheer scale of these deposits and their utility in modern industries. Unlike deep-sea nodules in the open ocean (e.g., the Clarion-Clipperton Zone), which require advanced technology to harvest, the Dead Sea’s minerals are relatively accessible due to its shallow depth (averaging 300 meters) and proximity to land-based infrastructure. This accessibility, combined with global demand for fertilizers, chemicals, and metals, underpins the economic hype. However, environmental challenges—such as the Dead Sea’s shrinking size due to water diversion—could limit future extraction, casting doubt on the full realization of such estimates.

In summary, the Dead Sea’s mineral wealth is a product of its unique geological setting: a tectonically formed, low-lying basin with no outlet, subjected to intense evaporation for millions of years. @RepThomasMassie @RealCandaceOImage 2. The Rothschild's purchased the land under Palestine before WW1 directly from the Ottoman Empire when they still existed.

They established the Palestine Jewish Colonization Association (PICA) in 1924, which acquired over 125,000 acres (50,586 ha) of land and set up business ventures. Most of you are ignorant of history.
Mar 30 4 tweets 5 min read
IVF doesn't solve infertility it bypasses Nature's laws that control the process. Modern humans have no idea how their tech world is causing it. They have created their own asteroid and I see it everyday in my clinics.

My Integrated Decentralized Narrative: From GOE to Modern Extinction
Let’s weave the dopamine circuitry findings into the evolutionary framework, highlighting how environmental light changes are affecting sex, fertility, and fecundity:

GOE (2.4 Billion Years Ago): Hypoxia and cooling favored the Warburg metabolism, with melanin degradation into L-DOPA providing dopamine for stress responses. Early mTOR-like pathways regulated growth but were not yet light-sensitive.

Evolution of Complex Life (Post-GOE): Neuropsin evolved, linking UVA light (380 nm) to mTOR and dopamine synthesis. Dopamine began regulating reward and movement, setting the stage for sexual behavior in complex organisms.

K-T Extinction (66 Million Years Ago): Darkness suppressed neuropsin and mTOR, reducing dopamine synthesis and shifting metabolism to glycolysis. Hypoxia increased catecholamine production, prioritizing survival over reproduction.

Post-K-T Mammalian Evolution: UVA light reactivated mTOR and dopamine pathways, supporting mitochondrial efficiency, circadian rhythms, and sexual behavior. Rhythmic dopamine in the vsNAc (modulated by acetylcholine) optimized ejaculation timing, enhancing fertility and fecundity in diurnal environments.

Primates and Humans: Dopamine in the vsNAc, driven by UVA light via neuropsin and mTOR, fine-tuned sexual behavior and supported sex steroid synthesis via CYP enzymes. This underpinned the evolution of complex social and reproductive behaviors.

Modern Extinction Event (Today): Reduced UVA exposure (from ALAN, indoor living) suppresses neuropsin, mTOR, and dopamine synthesis, leading to:
Quick Ejaculation: Dysregulated dopamine rhythmicity in the vsNAc causes premature ejaculation, reducing reproductive success.

Decreased Fertility and Fecundity: Impaired mTOR activity reduces CYP function, lowering sex steroid production and gamete quality. Intracellular hypoxia and mtDNA damage further exacerbate infertility.

Circadian Misalignment: Disrupted circadian clocks (via PER, CRY) impair dopamine and metabolic regulation, contributing to reproductive dysfunction.
Metabolic Regression: A shift to Warburg metabolism reduces ATP efficiency in gametes, impairing sperm motility and oocyte maturation.Image
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2. Predictions and Implications
Reproductive Health Crisis: The decline in fertility and fecundity, driven by light disruption, suggests a modern extinction event. Restoring natural light exposure (e.g., increasing UVA at 380 nm) would reactivate neuropsin, mTOR, and dopamine pathways, improving ejaculation timing, sex steroid synthesis, and gamete quality.

Therapeutic Interventions: SunLight therapy at 380 nm could enhance mTOR activation and dopamine synthesis, addressing ejaculatory dysfunction and infertility. Targeting acetylcholine-dopamine interactions in the vsNAc (as shown in the research) may also offer treatments for sexual dysfunction.

Environmental Solutions: Reducing ALAN and promoting natural light exposure could re-synchronize circadian rhythms, mTOR activity, and dopamine signaling, mitigating the reproductive and metabolic consequences of modern light environments.Image
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Mar 28 4 tweets 4 min read
Many things are impossible to centralized medicine.

When they say it, believe them.

It is impossible for them to do it.

But it is possible when your framework is not constrained by biochemistry.

Mainstream centralized medicine operates within a narrow biochemical lens: think enzymes, receptors, and pharmaceuticals, while largely ignoring the deeper physics of biological systems. Blue light damage to the eye, for instance, is a great example: they’ll talk about retinal degeneration or oxidative stress, but the conversation rarely touches on how light interacts with cellular water or electron dynamics. Centralized medicine tends to see these as "impossible" to reverse because their toolkit doesn’t account for the underlying mechanisms I pointing to.

My framework, though built on quantum mechanics and the biophysics of water, shifts the game entirely. The idea that water isn’t just a passive solvent but an active player, responding to temperature, pressure, pH, and ions like phosphorus, aligns with some cutting-edge thinking in biophysics.

Water’s coherent domains having structured regions where it acts almost like a liquid crystal, is obviously being used to be sensitive to salt levels and iodine, as a result, so is cerebrospinal fluid (CSF) because it is an ultrafiltrate of blood plasma.

The choroid plexus tweaking the chemistry of blood plasma into CSF is a solid observation; it’s a filtration system that’s more dynamic than most give it credit for. If salt modulates the physics of those coherent domains, I'm implying it would and should influence the brain’s redox potential, its balance of oxidation and reduction, which is a bold and provable claim. It’s like saying the brain’s electrical environment is tuned by water’s quantum properties. The physics says it is allowed.

The leap to “water electricity” powering cells and the universe is where I'm using physics to really push biochemical boundaries. I've suggesting for 20 yrs that sunlight-driven proton and electron currents in water, both inside cells and across extracellular spaces act as a photo-bioelectric messaging system for redox status. This isn’t far off from what some researchers explore with mitochondrial bioenergetics or the role of structured water in protein folding and enzyme function. Gerald Pollack’s work on the “fourth phase” of water, for instance, supports the idea that water near cell membranes can hold charge and drive biological processes. That work is supported by the work of physicists Preparta and Del Guidice. No one in biochemistry has any idea of this work, yet all their biochemicals only work if they are hydrated. That is their hypocrisy. I’ve been reversing diseases for 20 years using this lens by manipulating light exposure, hydration, or ion balance. It’s a testament to how practical this can be, even if it’s dismissed as impossible by the mainstream.

Centralized medicine’s paradigm doesn’t deny possibility out of malice; it’s just shackled by its own assumptions. They can’t “fix shit” because they don’t see the variables I'm playing with. My decentralized approach, open to probabilities and rooted in quantum effects, sidesteps those constraints.Image 2. @Charmd8888 reports significant vision improvement from 20/1000 to 20/400 in one month, defying her doctor’s claim that recovery from blue light-induced retinal damage is impossible.

Her approach aligns with my decentralized medicine model, using sunlight, red light therapy, and other methods i'd advocate for reversing such damage.

A 2023 study in the original thread confirms blue light (160 lx, 3–6 hours) collapses the inner blood-retinal barrier (iBRB) via claudin-5 degradation, supporting my biophysics-based explanation of retinal damage.

Red light therapy, as noted in a 2020 pilot study from the web results, can improve retinal function in people over 40, potentially by reducing oxidative stress and stabilizing tight junctions like claudin-5.

Charlotte describes her visual disturbance as a “beautiful intricate” pattern of purple-lavender with gold outlines, suggesting biophoton emissions or neural misfiring, which directly ties into my model of chaotic biophoton spread from retinal damage. Centralized medicine does not even know much less learn mtDNA transforms energy to light during mtDNA metabolism.

Her mention of the pattern becoming “smaller, lighter, and more transparent” indicates restoration and renovation of retinal coherence, likely aided by my protocol’s focus on light spectrum modulation and water coherence. Sounds like what Becker did in bone.

A cursory web search by an autodidact results in finding out that highlight cerebrospinal fluid (CSF) sodium rhythms peak in early morning and late afternoon, which would be expected to exacerbate retinal stress during those times, especially under blue light exposure. No eye doctor seems to know this. This is why renovation of the retina is impossible for them.

My quantum perspective on water as an electron and proton donor easily explains why Charlotte’s protocol likely involving hydration and light, Would should and could restore cellular redox balance in the retina.Image
Mar 24 16 tweets 13 min read
In 1860 Oliver Wendell Holmes, dean of Harvard Medical School, wrote that “if the whole materia medica, as now used, could be sunk to the bottom of the sea, it would be all the better for mankind—and all the worse for the fishes.” He was a prophet.

His Word are Historical Echoes to Modern Medicine: Just as mercury and bloodletting were standard in 1860, modern medicine has its own examples of widely used interventions later found to be harmful. For instance, the mRNA platform. Has killed more people in the USA than two World Wars. The advice you got from the Columbia Drug Cartels were better than Centralized medicine's advice. How about statins for high cholesterol because no one goes out in the sun any longer and is inside addicted to screens.

Opioid Crisis: In the late 1990s and early 2000s, pharmaceutical companies like Purdue Pharma aggressively marketed opioids like OxyContin, claiming they were safe for chronic pain. This led to widespread overprescription, addiction, and overdose deaths—over 500,000 opioid-related deaths in the U.S. from 1999 to 2020, according to the CDC. Like the toxic remedies of Holmes’ era, these drugs were pushed despite limited evidence of long-term safety. All because of screens and 24/7 LED lights that destroyed beta endorphin release from POMC.

Polypharmacy in Chronic Disease: Today, patients with chronic conditions like diabetes or hypertension often take multiple medications, often leading to adverse interactions. A 2019 study in JAMA Internal Medicine found that 42% of older adults in the U.S. were taking five or more prescription drugs, increasing the risk of side effects and diminishing quality of life. today the number is over ten Rx. BigHarma business model is a cartel for pseudoscience.Image 2. Can you fill a cup that is topped? Is a mind truly open if it is filled with facts that inconsequential? It is only when we are ready to give up on some things in our lives that we could receive new things. Unlearn to relearn today. Decentralize your thinking to leave the stagnation of centralized healthcare behind.

For instance, a doctor might know the exact protocol for managing type 2 diabetes with metformin but be unaware of how insulin resistance is influenced by environmental factors like blue light exposure at night, a concept Kruse frequently discusses. These "facts" are inconsequential if they don’t lead to better patient outcomes.

Diabetics have been managed on drugs for 100 years and the incidence and prevalence is not going down, it is getting worse.

No has a drug or supplement deficiency. The have a deficiaincy in their thinking.Image
Mar 21 12 tweets 9 min read
Patients navigating the highways of centralized medicine are on the road to nowhere and they're trying to escape. The escape route is through their environment.

THE SUN MANDATES IT. LET THERE BE LIGHT IS A TRUE STATEMENT REFLECTING A BIOPHYSICAL FACT. Every 150 million years, the Sun loses roughly the mass of Earth due to the solar wind, or about 30 Earth masses over the entire lifetime of the Sun so far. The whole of the living history of Earth, over 4.6 billion years, has consumed just 30 Earth masses of solar mass.

This volume shows just how much information is buried in sunlight. It also shows that DHA was critical in tapping the information in the light to make it useful. It explains why conditions of existence were and are more important than natural selection.

It explains the paradox of the Cambrian explosion from evolutionary theory. Light completes Darwin's ideas; DNA and genes do not. The Cambrian explosion happened 600 million years ago, and photosynthesis was innovated 50 million years before the Cambrian explosion.

When you divide 650 million years by 4.6 billion years, you will see that complex life found on Earth has only used 14% of the 30 Earth masses of sunlight. Around six masses of Earth created everything humans have ever known about life. THIS SHOULD FLOOR YOU. Everything ever created on Earth came from this amount of light. It shows us definitively how much more critical light is than anything else. However, to use this small amount of light, photosynthesis had to innovate DHA to make the sun's helpful light 600 million years ago. This shows you just how powerful the electromagnetic force is. It has unlimited range and power. DHA has been the master of DNA since the beginning of animal evolution because it made light useful from an information theory. It explains why I believe Darwin was very wrong. CITES threadreaderapp.com/thread/1894822… 2. The rise of entropy in aging is inevitable but negotiable. My tweak is that entropy isn’t just éR or ROS/RNS; it’s the loss of mitochondrial fractal coherence, where IMM potential (ΔΨm) frays under nnEMF and hypoxia. Graceful agers don’t deny this; they adapt to it. Photobiomodulation (PBM) restores ΔΨm by 20-30% (per Hamblin’s work), while methylene blue (MB) shunts electrons to Complex IV, cutting reductive stress. Our rejection of cosmetics or melotan for bioenergetics is pure savagery because sunscreen blocks UV-A’s mitochondrial benefits, and sunglasses kill melanopsin signaling. My tribe won't do dumb shit like this below.Image
Mar 15 4 tweets 3 min read
Every mental disease is on an energy spectrum.

Not realizing this is part of why centralized medicine needs to be extinguished. 2. How does it happen? Simple.......Read this book first. Assimilate the lessons in it. Image
Mar 15 19 tweets 14 min read
1. We are the product of stardust that has burned us using oxygen. It light is the anvil which forged me which gave the will to make me formibile for my misfits because I will not break under force. All living things are electric and magnetic and they use the electromagnetic radiation of the sun and the earths magnetic field to create life. Man made radiation disrupts the natural order of atoms in our cells. The electromagnetic signals that come from the organization of these cells in mtDNA creates our health span or chronic diseases epidemics. This is plants and animals.

Humans are diurnal animals who need sunlight and darkness after sunset to function. This makes them fully decentralized. They cannot be optimal with too much of either. Indoor living, sun avoidance, constant exposure to artificial lights and man made electromagnetic radiation = a shifted metabolism from light that leads to all chronic diseases. Optimizing melatonin, dopamine, and melatonin (sunlight/darkness) and solar derived vitamin D, melanin, and NO is how you avoid chronic disease.Image 2. Life as Electric and Magnetic: The Stellar and Terrestrial Forge

My assertion that “all living things are electric and magnetic” aligns with the decentralized photo-bioelectric framework I’ve been building for 20 years:

Stardust and Oxygen: The elements forming us—carbon, hydrogen, oxygen, nitrogen—originated in stars via nucleosynthesis, later dispersed by supernovae. Oxygen, became abundant after the GOE (~2.4 billion years ago), became a “burning” force, driving oxidative stress but evolving and enabling aerobic respiration. This “anvil” forged life’s resilience, by necessitating adaptations like mitochondria and structured water to manage “electrocution” of the atmospheric change of the GOE.Image
Mar 14 23 tweets 19 min read
My view is that it is all quantized to electromagnetism, the structure of elements on the periodic table, and how they vary their physics as the environment changes on Earth. This scales to the mathematics of size and shape which is a thermodynamic idea and ultimate it ends up with the idea linking to Platonic solids. I have a non Darwinian approach.

My non-Darwinian take could argue that climate tensions (cold, dry) imposed thermodynamic constraints—say, energy budgets forcing molecular efficiency—that “snapped” haplotypes into new forms, bypassing random mutation. Think of it like a system finding a lower energy state, not trial-and-error survival.

But Darwin’s model still holds up because there is a memory of the past in cells: ancient DNA shows gradual haplotype shifts in humans (e.g., lactose tolerance in northern pastoralists), not sudden jumps.

Quantum mechanics might tweak mutation rates (e.g., UV damage to DNA), but it’s not replacing selection. It does argue that gradualism is not the key. Timing and thermodynamics are the key.

Why do I run with this anti-Darwin angle in my work? Consider the Cambrian and K-T suggest environmental jolts—like climate swings or impacts—could trigger rapid, physics-driven reorganizations.

Maybe this answer I am giving you sees human migration similarly: a climate shock flipping genetic switches. It’s intriguing, speculative, view point of decentralized biology that still leans on selection to explain haplotype patterns, even if physics sets the thermodynamic stage of adaptation. 2. My view is that Darwin was wrong to focus on natural selection as the primary driver of evolution, missing the deeper role of quantum mechanics and thermodynamics.
I highlighted:

Hemoglobin Variability: Birds (e.g., Arctic tern) and reptiles (e.g., alligators) show extreme hemoglobin adaptations—high-altitude flight versus underwater hibernation—that Darwinian gradualism can’t explain. I suggested these reflect quantum-driven leaps tied to environmental conditions, not slow selection.

Conditions of Existence: Darwin emphasized this over natural selection but couldn’t explain it. I equate it to epigenetics, driven by quantum field physics (e.g., light and energy interactions), not random mutation.

Quantum Thermodynamics: Evolution operates via mass equivalence (Einstein’s E=mc²), where energy quanta shape biological forms. Morphology (Darwin’s focus) is secondary to these physics-based mechanisms.

Critique of Neo-Darwinism: Figures like Dawkins cling to natural selection without a molecular mechanism, ignoring Feynman’s call for precision and Einstein’s insights into energy. Genes are not deterministic.

Light as Driver: Information in light (e.g., electromagnetic forces) controls life’s direction, a quantum process Darwin couldn’t fathom in his era.

My view is that evolution isn’t a gradual, selection-driven process but a series of quantum jumps triggered by environmental energy states—think thermodynamics and light, not survival of the fittest. It is a survival of the wisest in information processing.

I wrote this 19 years ago and posted it 111 years ago on the topic and my opinion still has not changed.

jackkruse.com/osf-3-darwin-w…
Mar 10 6 tweets 5 min read
Remember when Danny Jones asked me at the end of our first podcast why all the young males he knew were taking testosterone and wanted to know if this was somehow related to the MKULTRA story, and I smiled?

Well, it is.

The Great Oxidation Event, what I like to call the Oxygen Holocaust due to nnEMF toxicity, is going on in every skull on Earth now due to nnEMF and blue ubiquitous use.

Suppose you understand what I have laid out on my blogs over 20 years. In that case, all chronic diseases are photo-bioelectrical electrocution of the inside of a cell of the anterior pituitary and the gonads by cell phones in the pocket next to said jewels is ongoing.

Why? Dehydrated melanin causes massive amplification of the DC electric current a cell makes. When you dehydrate cells of water, it also increases the amount of NaCl left behind, which increases the chance of stray electrical current spreading where it should not be. Your anterior pituitary and your balls. This is why those affiliated with DARPA and the FDA just did this.

Centralized MDs will run to write Rx for BigHarma. My tribe knows better. If you knew how to ask better questions, you'd discover that the ionosphere is a giant RF microwave device that dehydrates you daily. @JonesDannyImage 2. The blue light man has made via the MKULTRA experiment, which is now global, will destroy this heme cytochrome by vitamin A liberation. NO = Nitric oxide is also destroyed.  Recall that NO controls the behavior of our stem cell depots.  This is why every snake oil salesman now sells lemmings stem cell injections.  Moreover,  I hope you remember the lesson I delivered in Patreon: this information carried in NO concentrations is also supplied to the POMC/melanin complex in cells when hemoglobin is in a specific oxidation state.  Melanin has to be well-hydrated to optimize any hormone panel at the brain and gonad level.  Right now, nnEMF is causing a TBI in everyone's anterior and posterior pituitary (vasopressin) while causing mtDNA mutations to diminish DDW production at cytochrome c anther heme-based protein.

380 nm light also controls the regenerative state of your hormone panel. This was a tremendous optical arrangement for the survival of mammals 65 million years ago. Still, it is now a big problem when you realize that we are in the Great Oxygen Holocaust due to nnEMF and what dehydration of the heme-containing cytochrome P450scc is designed to do in modern mammals' insides under the power of ALAN, where POMC is boss.

This enzyme carries out the so-called side chain cleavage reaction, consuming cholesterol to produce pregnenolone, the precursor of cortisol, and all other steroids. If melanin is not well hydrated, this cleavage fails, and you get pregnenolone steal syndrome.  This is why males are losing testosterone at record rates and why females' sex steroid hormones are being demolished too.

Glucocorticoid synthesis is tightly regulated at the level of cholesterol metabolism, which responds to ACTH stimulation over minutes and ceases equally quickly when this hormone is removed. All require well-hydrated melanin sheets to make Becker's regenerative current.  Remarkably, this dynamic process is modulated under most circumstances not by control of the intrinsic enzymatic activity of P450scc, but rather by substrate availability. If that substrate is not there because you're missing Becker's current you are screwed.  For this reason, cholesterol transport within the mitochondrion has emerged IN ALL MAMMALS as the key control point for steroidogenesis.

Epigenetic light signals control all your hormone panels.  MKULTRA found this out in 1964, and the government has weaponized it to put in screen technology to use against you since screens replaced paper.  It was confirmed in Neil Armstrong's testosterone catastrophe when he returned from the Moon.  Not only did he have pseudotumor cerebri, but he also had head optic nerve swelling that linked his nnEMF exposure to his acute rapid loss of pituitary function.

DARPA took the lesson and added to another silo they developed in California where screens were moved from green analogy signals to blue lit.  This is why books are being cancelled for screens, and all screens are now all blue-lit. It is why Obama and Biden are burying incandescent bulbs from markets—the implications of the Danny Jones podcast are on display in this very post. Few will make the connections. Thankfully, I am interested in those who will.

Science is a tough place not to get canceled these days.Image
Mar 10 9 tweets 4 min read
How did we get creativity? Neanderthals migrated North got to 51st latitude froze started wearing animal skins and used fire inside caves and their brains shrunk as a result. As they shrunk due to dehydrated melanin sheets, melanin becomes dopamine. The dopamine built up and we got art culture and DaVinci.Image 2. Note how melanin degrades on the slide on the top line. It degrades into dopamine, other amines, and L-DOPA. When you undergo a TBI, as the Neanderthals did by going too far up on the planet, it gets cold, and you need animal skins and fire to keep you warm. Why? Neanderthals did not have uncoupled haplotypes yet. That is a human innovation to high-latitude living. As a result, they flood their shrinking brain with more dopamine than they should have had. Voila = You eventually get Michealangelo, DaVinci, and Rembrandt.Image
Mar 9 13 tweets 13 min read
The Birkeland currents in space directly scale to the bioelectric currents and electric resistance on our membranes in a cell, so yes this post is spot on. Image 2. As Chris points out, Birkeland Currents are observed in Earth’s magnetosphere (e.g., 10⁵-10⁶ amperes), these currents are driven by magnetic reconnection, a process scalable to cellular ion channels. No direct studies link them to bioelectric currents yet but maybe @MitoPsychoBio or Levin will consider testing this as Becker did with Brown in the UK, but fractal models (e.g., 2022 Physical Review Letters) suggest universal energy flow principles because these are laws of nature not subject to belief.

Space Weather and Health: A 2023 study in Scientific Reports correlated geomagnetic storms with increased hospital admissions for mental health issues, supporting the bipolar disorder claim. Anthropogenic nnEMF (e.g., 5G at 3.5 GHz) is understudied, with the WHO citing insufficient evidence of harm, possibly due to industry influence.

Melanin and Bioelectricity: Becker’s work showed melanin conducts currents (e.g., 10⁻⁶ A/cm² in salamanders), disrupted by dehydration, aligning with my ideas here. Sunlight’s role in melanin hydration lacks large-scale data but fits the physics that underpins chronobiological evidence.Image
Mar 9 37 tweets 32 min read
1. The world is an energy vampire built by technocrats/DARPA to drain the brain of energy to propel us to proper actions We can see this blueprint in peole with bipolar disorder. How does a decentralized MD see this disease that centralized psychiatrist have no answer for? Image 2. Bipolar disorder (BD) is a chronic and common psychiatric pathology, which can be particularly disabling. The disease has a global prevalence rate of 1–4%, begins at an early age, i.e. predominantly between 15 and 25 years old, and persists throughout the life of patients. BD is characterized by a recurrence of mood depressive episodes (pathological decrease in mood and energy), hypomanic or manic episodes (pathological increase in mood and energy), or even mixed episodes (simultaneous presence of depressive and manic symptoms).

These thymic episodes are interspersed with phases of clinical remission, known as “euthymic” episodes. The disease is associated with a high morbidity and mortality rate and due to the significant functional impact it induces, including during euthymic periods, BD is the cause of poor quality of life and is one of the ten most disabling diseases according to the World Health Organization.

The diagnosis of BD is mainly clinical and can be supported using scales or questionnaires. The diagnostic delay is estimated at around 10 years. This delay is clearly related to the heterogeneity of the clinical expression of the disease. The study of the literature shows that this delay in treatment seriously affects the prognosis, particularly on the functional level, and constitutes a major public health problem. In addition, there are no biomarkers, easily usable in current practice, to help the clinical decision for the diagnosis or for predicting the course or prognosis of the disease.Image