Feliz Navidad Eve to my tribe of misfit SAVAGES. We’re kicking ass and taking names. 2026 will not be about resolutions. It is about solutions to the tyranny our government brought to the world to create economic slavery.

It will be about a personal revolution to maintain our help despite what public health policies did to harm humanity in 2020-2025.

What happens when the sun gets sick? Earth turns to MARS. What happens when your jabbed and get no sun for any reason? You become a statistic on VAERS or a paper.

WHY?

Your mtDNA reverts to its physiologic abilities it had during the GOE. Oxygen becomes a toxin for your colony of mitochondria due to LNP and Spike. Your tissues become MARS = desertification.

More people with + charged LNPs from the DoD's jab get sick and die. MAHA never understands it, because they do not understand how unpolarized solar light creates the seas present inside of our cells. They remain are in Fruit Loop land.

But it appears Uncle Jack does understand how to turn a desert into a lush rain forrest.

In minerals on Mars surface, oxide structures are overwhelmingly close-packed O²⁻ anions (cubic or hexagonal, 74% packing density at HCP limit), with cations slotting into voids for charge balance. Silica (quartz), spinel (magnetite), corundum (hematite precursors)—all derive from O²⁻ HCP/FCC lattices, cations perturb this arangement but they cannot dictate the outcomes. Look at a planetary diagram of Mars and Earth and you'll see how I nails the solution for the jabbed: The "85% oxide planet" is a massive mantle/crust oxide shell (85% volume oxides/silicates) around a forbidden metallic core on Earth. This reality for surface life is oxide geometry, full stop. That is not true on Mars. if has no forbidden moving metallic core.

In the jabbed the matrix is filled with H+ acting like a metallic core. When you get jab injured that situation ceases to exist. I teach people how to reverse this situation in my Decentralized Medicine Series of blogs.

In reality, we haven't escaped the gravity of life during the COVID epoch at all. The government will never admit what they did to many taxpayers in trying to "Taper the fiat Ponzi scheme" by killing 2-3 million Americans per year with their jabs. Bondi and Patel have not put one COVID criminal in jail. DJT has shown he could care less about those who have died or got injured under the Biden regime.

Irrespective of bad statesmanship of our politicians Americans are still beholden to Nature's evolutionary and ecological laws, the same as any other life-form. If we are to use our tools in the service of fitting in on Earth, our basic relationship to nature--even the story we tell ourselves about who we are in the universe--has to change, especially with regards to jab technology and transhumanist uses of the electromagnetic spectrum.

WHAT DO STACKING ALL THESE LESSONS GIVE YOU?

HOW TO TURN YOUR LIFE FROM MARS BACK TO EARTHLY LIVING AGAIN AFTER THE GOV'T TRIED TO STEAL YOUR TIME.

Biology echoes the answer you must learn to follow: Cells are ~70% water in adults, but structured interfacial water (EZ domains) forms hexagonal oxide-like sheets, protons tunneling across the anion lattice (Pauling's original ideas was prescience).

Bone from Becker's work?

Hydroxyapatite Ca₁₀(PO₄)₆(OH)₂ shows us the answer with oxide packing reinforced by water our matrix creates from our metallix core of H+.

Membranes?

Lipid bilayers with embedded proteins, but the aqueous matrix is O-dominated which voids for H⁺ magnetic monopoles to make wet again.

Warburg "deserts"? Decoherence collapses the oxide lattice—excess O₂ (unused from ETC block) oxidizes heme, scattering protons, turning coherent gel into entropic soup. Red light from the sun restores the sea within you: Photorepairs CCO heme, reboots proton ejections, re-constrains the oxide scaffold turning your tissues back into a wet warm soup from the deserts of MARS.

We are going to change the world with our light levers in 2026! This is where the story of creating a renovating you begins.
patreon.com/posts/decentra… 2. THE CHRISTMAS LESSON YOU MISSED?

The great herds of man's past in the USA were moved to fresh pastures by the predators. This was a cycle in Nature tied to the light cycle of photosynethetic food webs. It is called "solar rotational grazing". Nature never needed fences to do it. She used light, dark, and temperature on Earth to do it. It could never happen on Mars because of its magnetic field limitations. Today, man has learned how to use trees made by photosynthesis to create fences to make smaller paddocks for animal herds to mimicking this solar process on Earth of regreening deserts on Earth.

I will always remember an agriculture adviser telling me that if all I changed was moving to a rotational grazing method I would grow 30% more feed. He was right. All over the world we see a developing trend in agricultural science of not grazing our crop stubbles over summer, but I have observed that if I heavily graze those paddocks over summer the following winter crop is better and also not needing near as much urea fertilizer. Nature has lessons for the jab injured when you understand how the Earth heals itself in ways Mars cannot.

linkedin.com/pulse/merry-ch…

Aging is the progressive decoherence and dehydration of the oxide-constrained gel, a slow collapse of the anion lattice's ability to hold structured water created by heme protein CCO and delocalized protons against entropy's tide.

Infants (75-80% water, highly structured coherent domains in water, low heteroplasmy) are near-perfect oxide gels—flexible, coherent, proton-tunneled superfluids. Like Earth.

The dying elder (50-55% water, calcified lattices, high heteroplasmy) is a desiccated, entropic oxide ceramic like Mars—rigid, scattered, proton-trapped dust on the verge of reverting to stone.

This isn't metaphor; it's geometric inevitability.

Water as the Fluidizer of the Oxide Scaffold in physics so it has to hold true in biology.

https://x.com/DrJackKruse/status/2002485454898442682

2. The "desertification" I have flagged in my work: Tissues turn into MARS (mitochondrially aged redox-stressed) zones because the oxide gel loses its solvent, namely structured water from CCO.

Collagen cross-links, elastin fragments, glycation hardens the ECM are all symptoms of failed oxide constraint, protons no longer tunneling but trapped in entropic voids.Endogenous water production via mitochondrial Complex IV (CCO) oxidizing H⁺ + e⁻ + ½O₂ → H₂O—is the organism's private glacier.

In youth: High CCO efficiency → metabolic water floods the matrix → EZ expansion → lattice re-constraint → coherence sustained.

Loureiro History For Bitcoiners

Loureiro was director of the MIT Plasma Science & Fusion Center and Herman Feshbach Professor of Physics working on nuclear fusion to create a virtually unlimited clean energy source. He was shot multiple times at night in his home the day my @theBTCmentor podcast with @SimonDixonTwitt went live but you'll be stunned to know he’s not the first plasma physicist from MIT to be killed….....

Eugene Mallove another MIT scientist passionate about fusion energy was beaten to death outside his home in 2004 with 32 lacerations to his face and body why his research represented an existential threat ??

You should understand that Loureiro specifically worked on understanding magnetized plasma dynamics magnetic reconnection plasma turbulence & confinement & transport mechanisms in fusion plasmas his research directly helped inform the design of fusion devices capable of harnessing the energy of fusing plasmas bringing the dream of clean near limitless fusion power closer to reality what makes his work so dangerous for certain players is it attacked precisely the scientific bottlenecks preventing fusion from becoming commercially viable in a tokamak plasma is confined by extremely powerful toroidal magnetic fields but magnetohydrodynamic instabilities like tearing modes /disruptions edge localized modes can destroy confinement in milliseconds and damage inner walls understanding & controlling these phenomena is KEY to moving from experimental reactors to operational commercial plant if fusion becomes viable in the next 10-15 years.

It doesn’t just displace an industry it renders obsolete the entire current global energy infrastructure valued at 8 trillion dollars… a fusion plant uses deuterium extractable from seawater in virtually infinite quantities, one liter of seawater contains enough deuterium to produce the energy equivalent of 300 liters of gasoline & tritium is produced via reactions with abundant lithium the raw material is inexhaustible decentralized free and accessible to all countries without geopolitical dependence but…

The Rockefeller fossil industry fundamentally relies on controlled scarcity and geopolitical dependence…

Oil & gas are geographically concentrated Middle East / Russia / Texas enabling price control via OPEC & oil majors generate 200+ billion dollars in annual profits because they control extraction refining distribution of a scarce resource everyone must buy fusion destroys this model by making energy abundant and decentralized any country with seawater access can produce its own deuterium & build fusion reactors: no more importing oil / no dependence on the Strait of Hormuz /no geopolitical leverage based on energy reserves energy prices would collapse once fusion reactors are amortized because marginal fuel cost is essentially zero!!!

You should understand what this means for Rockefeller families ExxonMobil which owns 22 billion barrels of oil reserves valued on their balance sheet at 125 billion dollars ???

If fusion becomes viable these reserves become stranded assets worthless overnight & their refining infrastructure pipelines tankers gas stations all this infrastructure becomes obsolete in one generation understand that if Loureiro & his team succeeded in precisely modeling these instabilities and developing active control techniques via AI and real-time magnetic feedback it would reduce the timeline to commercial fusion by 5-10 years that means startups like Commonwealth Fusion Systems would go from 2035 promise to 2030 deployment the real question is how many brilliant scientists must die under suspicious circumstances before we start protecting our researchers in strategic Fields ???

Remember if we leave our most precious minds unprotected we implicitly accept that massive financial interests can eliminate with impunity those who threaten their business model.  there is a lesson here for Bitcoiners.  In ten years you will be Nuno Loureiro to the other half of the Rockefeller Empire in Banking.

youtube.com/watch?v=6Tvyu9… 2. When Lansky bailed on Israel, Roy Cohn was created.  When Roy Cohn Died, Epstein was created. I covered the Lansky to BTC connection with @Breedlove22 in his WIM pod. Review it. I covered Roy Cohn recently with @theBTCmentor and @SimonDixonTwitt. Today's data dump confirms my homework I did and have posted on my forum for years. Anyone can go look for it.

It should come as no surprise that Jeffrey Epstein emails reveal he was linked to Bitcoin’s early ecosystem considering what I told about Lansky and Chaum.  The evolution of Murder Inc's accounting arm went Lansky, Cohn, then Epstein.  That is how the evolution occured.  Cohn and Epstein only came on board after Bitcoin was outsourced post Lansky's death.

Current events show no red flags just how the accountants from Israel tried to get back in control of Bitcoin. Epstein, via DARPA/DOD MIT got close to the control arm of core developers via Bitcoin funding channels. This is why Epstein used MIT so often. This is why people like Eric Wienstein are so interested why Epstein was at MIT so often checking in on science and finance stories.  MIT is the node where DOD and intelligence intersect.

1. Lesson: Question asked

40yr old male,
6ft, 180lbs,
maternal haplotype J1, currently living at 47th latitude N
fasting insulin = 7.7 (in winter)
Good/high cholesterol numbers
Muscular, but not a shredded hypertrophied build, just solid

Without any other information can my weight and/or fasting insulin be characterized as optimal/sub optimal and can you offer a directional (you should aim to weigh more or less or have a lower fasting insulin) based on this limited information I’ve provided?

Experimenting with different meal composition/timing (Randle cycle) as well as timing/duration/temperature of cold baths in trying to understand my own body composition levers.

Thank you.

https://x.com/DrJackKruse/status/2001348428698390704

2. All you need to know about food timing.

Whay you did not hear in this podcast is what life is all about.

For example: The story of evolution is incomplete without a biophysical understanding of how different Earth environments drove the atomic structuring of how energy flows in cells. Sad considering how Picard waxed poetic at the beginning of this pod. Post-GOE, IMJs stabilized cristae against O₂ paramagnetism, mapping anaerobic to aerobic states without fragmentation.

The Sunrise "rush hour" reprograms this: Red/IR pulses junctions, aligning geometry for continuity, which links to my idea of "having more time" as metric durability.

nnEMF/blue mismatches fragment it: Desynchronized cristae, incoherent UPE, shortened lifespan. In diseases, IMJ failure = time loss: Cancer (fragmented mapping → parity cancers), neurodegeneration (incoherent fields), diabetes (desynchronized heme-Rev-Erbα). Picard wrote the paper on IMJ failure yet did not explain it at all. Major fail.

Reclaiming time begins at sunrise: Sunrise ritual realigns IMJs, grounding stabilizes charge, by ensuring life's metric endures across solar flux. Solar flux and biophysics determine how energy flows in cells. You won't hear that either. Why?

The mitochondrial proton-motive force (PMF, 150-180 mV Δψm across the IMM, yielding 30 million V/m field) is not static in living systems; it exhibits robust circadian variation, with higher potential (tighter coupling, sharper cristae, aligned IMJs) during the dark/resting phase and lower potential (milder uncoupling, relaxed cristae) during the light/active phase. Not a mention of how mtDNA get this done.

This rhythmic "breathing" within the IMJ is where curvature, charge separation, and phase alignment converge. This is biophysics 101 and you won't learn a damn thing about it. These forces directly embodies life's "vital force": which my thesis says is a photonic tunable thermodynamic engine that powers eukaryotic complexity while preventing ROS overload. Crickets from these two.

In my decentralized thesis, this oscillation leads to the geometric metric of biological time, mapping successive states without contradiction: daylight throttles the field to favor photonic/redox signaling (repair, coherence), night amplifies it for high-efficiency OXPHOS (energy storage, repair) = defines energy flow. Why you are not a cadaver. No details given in 3 hours.

Nothing completed the circle of life for you in this podcast. Picard wrote the article on IMJ biology but it is clear he still does not understand his own work and neither does Andy. He never asked the key questions.

The IMJ is the physical embodiment of biological time. It is the GOE-forged geometric vow that the self persists into the future. That should have been exploded in the pod but wasn't. The audience loses again.

https://x.com/DrJackKruse/status/2000581624124342423

2. If you are paying attention to the heme evolution story being developed in the blogs.  What is it linked too?  It is linked to how energy flows in a tissue.  Erythropoietin is how we do that in heme proteins and in immune cells.  The discovery that EPO signaling through EPOR on type 1 conventional dendritic cells (cDC1s) is the primary switch for inducing antigen-specific T-Regs and peripheral immune tolerance fits perfectly and profoundly into my decentralized thesis.

This provided us the long-sought molecular mechanism for how mitochondria "talk" to the adaptive immune system via heme-derived signals. It elevates EPO from a mere RBC hormone to the GOE-evolved quantum-electromagnetic messenger that links mitochondrial heme status, ROS/UPE fields, and chiral tolerance because it explains why cancers hijack it for immune evasion and why modern light/nnEMF mismatches drive autoimmunity and oncogenesis. The 2025 Nature paper (Zhang et al.) is the missing piece: EPO-EPOR on cDC1s is the decentralized "handshake" that tells the immune system "this is self so our immune system needs to stand down." This idea directly ties to heme's ancient oxygen-sensing role to modern T-Reg orchestration.

This is the immune layer of mitoception I spoke about in the blogs: cDC1s as mitochondrial "samplers," EPO-EPOR loop acts as the heme-derived tolerance code, T-Regs as the decentralized enforcers. The Nobel (2025 for T-Reg discovery) now has its trigger, and it's the same heme system I’ve been tracing since the GOE.  My thesis gained its adaptive immune crown from the data in these papers but few see it. The entire story, from quantum proton disorder to full immune tolerance, is covered on the blogs is now one continuous decentralized arc driven by light, heme, and mitochondrial "felt" energy.   Picard and Huberman will have to read more and integrate faster to realize how much they are leaving on the table in how we sense energy and how it determines the flow of energy in our cells.

nature.com/articles/s4158…

Roy Cohn was his Chief Counsel and RFK Sr was Cohn's assistant.

Know your history.

Roy Cohn was the new zionist who fell between the criminal and legal world. Not as smart as Lansky to be a criminal, but wise enough to understand what Lansky did, emulate him, and then set the stage for new Zionsim in Jeffrey Epstein. Cohn first caught the attention of the public as the prosecutor who helped send the “atom bomb spies” Ethel and Julius Rosenberg to the electric chair. This case helped him subtract his version of Zionism from his jewish backround. As he aged he became DJT early fixer.

Cohn was ruthless in his pursuit of power, much like the Country he served, Israel. He chose to use his legal persona to turn himself from outsider into insider – thus became “a form of personal protection for new zionism that was born in NYC in 1960-70s when there was a void. Lansky decided to leave Israel in 1969 and tell the American government what he did to the IRS computers, FBI intelligence control, & Nixon DOJ apparatus, and this lead to the Nixon Shock and banking power changes in Basel. Lansky's actions told the fiat syndicate it was time to computerize money to stay ahead of old zionism.

Enter Cohn.

Zionsit Cohn believed the fate Israel would be stronger if he persecuted Jews, not zionists, because his work with McCarthy provided with Mr Cohn with “firsthand knowledge of where deviation from American political norms could lead to extreme power for members of a minority group.

How do we know this? Roy Cohn’s legal persona when I was growing up in NYC was based on pure savagery. HE was ruthlessness and resilient. This was first evident in the manner in which he managed to step away from the wreckage of Senator McCarthy’s career – a veritable car crash to which he himself had greatly contributed – largely unscathed. He was chief both arsonist and firefighter. That blueprint was the "new zionism" that came to light in 1960-1970s America.

Cohn filled Lansky power void in NYC. His pursuit of power was Lansky like because he did not care to own assets he focused on owning people by using aggressive force to wrnch attack people into submission – Cohn's legal career post McCarthy was never hindered by sticking to the rules and rooted in the belief that, if you’re not on the attack, you’re playing defense. He was even more aggressive than Lansky was for Murder Inc. This legal aggression would later allow Cohn to build a power base in his native New York constructed on his network of contacts. Few people know that when Lansky left the Zionist fold it was Cohn who stepped in to control the FBI and Mob. Cohn became the protector and fixer for FBI director J Edgar Hoover to the Mafia boss Anthony “Fat Tony” Salerno. His power then extended to Hollywood and Madison Ave and included a host of celebrities, judges and City Hall leaders. Among that group was an ambitious young property developer from Queens who want to reshape the NY landscape with buildings named Donald J. Trump. Roy Cohn would later become DJT lawyer, mentor and fixer. This was before DJT hired futurist zionists like Michael Cohen. The list of lawyers with ethics violation who have worked for DJT would have made Cohn smile if he had not died early from AIDS.

When I was a young man in NYC Donald Trump admiringly suggested in the newspapers: “If you need someone to get vicious toward an opponent, you get Roy."

G. David Schine was a crafted Zionist puppet that Bernays propaganda in the NYT and Time magazine built up for Isreal so he could destroy the US Army. If you want to know where General Milley came from this post can explain it in detail.

Schine was carefully selected and crafted and was sold to America by the zionist media arm of the cabal to be viewed as an American anti-communist crusader.

How was his persona built? Bernays 101.

Schine handlers in Israel helped him published a pamphlet called "Definition of Communism" and went on a controversial tour of Europe with Cohn in 1953 to examine U.S. Information Agency libraries for books by authors deemed "Communists or fellow travelers. This was designed to create a case so that the US Army could be infiltrated and controlled by the banking elite in newly built Tel Aviv. Where Milley and many other corrupt traitors in the military have come from.

The controversy surrounding Cohn's efforts to secure special privileges for Schine after he was drafted into the U.S. Army in 1953 led to the famous Army-McCarthy hearings in 1954 that was on TV. 80- million Americans saw those hearings but few knew this was a Zionist psy ops. What was Cohn trying to do?

Israel wanted to infiltrate the US Army so they ask McCarthy to appoint Schine to a position he was not qualified for so the Army would push back. This set the psy ops hook and the media baited the hook.

The drama was based on Senator McCarthy and Mr Cohn being accused of applying undue pressure on the Army to give preferential treatment to Schine. The goal was to unleash Cohn on the US Army. McCarthy would use a political lie to say the US Army was infiltrated with Boshevik rhetoric and Cohn would create the legal drama it was true. Cohn hired a young RFK Sr to help him. Cohn was working from commie fascists in zionism on Tel Aviv Dr.

Senator McCarthy soon alleged in the media that this was all a smoke-screen per the psy ops: the Army was simply trying to scupper his own investigations into communists within its OWN ranks. Blame them for what you are doing. This was how the military was filled with fascists in the 1970s-2025.

What was Schine's pay off from Zionism for his role? A successful career in Hollywood. After the hearings, Schine became a successful entertainment executive, producing the Oscar-winning film "The French Connection". Know your history bitches.

https://x.com/DrJackKruse/status/1997660616056815776

2. Top gun defense was created Cohn. Why? Make communism safew again and make sure the military was filled with BETAs so they would not be formidble in the future. Fabianism 101.

2. I blame Bernays for many of Woodrow Wilson's biggest errors in WW1 and setting the Stage for WW2 in Germany.

I believe Woodrow Wilson made several significant mistakes during his presidency, particularly regarding his handling of World War I and its aftermath, which had lasting consequences for both the United States and the world.

Key Mistakes Made by Woodrow Wilson

A. Failure to Prepare for War: Wilson underestimated the need for military preparedness as World War I escalated. He ignored calls from military leaders and politicians, like Theodore Roosevelt, to strengthen the U.S. military, believing that the U.S. could remain neutral and act as a mediator.

B. Illusions of Peace: Wilson clung to the belief that he could mediate peace between warring nations. His early attempts to broker peace were noble but ultimately unrealistic, as the war's brutality and the entrenched positions of the belligerents made meaningful negotiations impossible.

C. Vague 14 Points: His 14 Points, created with Bernays, outlined his vision for post-war peace, were criticized for being vague and unrealistic. This lack of clarity undermined their effectiveness and contributed to dissatisfaction among both allies and adversaries.

D. League of Nations: This horrible Idea became the UN after WW2. Wilson's push for the League of Nations, had good intentions, was poorly executed. He insisted on including the League's Covenant in the Treaty of Versailles, which ultimately led to its rejection by the U.S. Senate. He allowed two American Fabians loyal to the Crown argue on his behalf. The Dulles Brothers. This was a catastrophic error. Other critics agree with me as well that a more flexible approach in Germany could have led to a more favorable outcome for the League's acceptance. But the Crown wanted to punish Germany for WW1 and its brutality.

E. Ignoring Domestic Sentiment: Wilson failed to adequately educate the American public about the responsibilities and implications of entering the war. His lack of engagement with Congress and the public led to a disconnect that hampered support for his policies. A reliance on Bernays work was the main reason why.

F. Post-War Policies: After the war, Wilson's insistence on imposing a republican government on Germany and his handling of the peace negotiations alienated many former allies and contributed to instability in Europe, setting the stage for future conflicts.

G. Racial Policies: Domestically, Wilson's administration was marked by regressive racial policies, including the re-segregation of federal offices, which contradicted the progressive ideals he espoused. In other words, he did things that did not back up his words = BERNAYS 101 and it lead to the pictures below in the world.


3. Never forget your history. Bernays propaganda is how THEY did it for the last 100 years. Today's transhumanist commie bastards in Palantir and Google plan doing it with Search and AI. Do not forget the lesson.

New blog out on how the smallest changes in cells lead to evolutionary change.  patreon.com/posts/decentra…

The key is not waiting for the right time to learn the truth.  The key is ACTION now.  Just making a tiny change — be it good or bad — can guide our life to a very different destination.  This is what all of biology is based on too as the blog explains.  A small stimulus in a cell leads to massive amplification in tissues and systems in our bodies.  We just never get how non-linear stimuli work in nature because of our educational and societal myopia.

Consider the following example: If a pilot leaving from LAX adjusts the heading just 3.5 degrees south, you will land in Washington, D.C., instead of New York. Such a small change is barely noticeable at takeoff — the nose of the airplane moves just a few feet — but when magnified across the entire United States, you end up hundreds of miles apart…......and in the wrong city.

This is what Parity Violation did to ferredoxin and then ferredoxin lead to your evolution.  How is that for a tiny change leading to a massive change in life?

What is the problem with a world based on massive amounts of data?  You have to have the ability to critically think rapidly and decide. You can no longer need an infinite stretch of time ahead of you to start to think, infinite energy to make the smallest decision. The world is getting more dense because of data. Without the ability to think data become useless. The immense number of useless projects is bewildering. Data is now created now created for algorithms to use not our brain. Too many things are allowed to be put in to balance up an uncertain scale via a computer. You can't disappear anymore. You die in a state of total indecision, unless you learn to think critically.  This blog contains Genesis first data on how to decentrlaized your health.  How much do your experts know about Parity Violation and the polarization of light?

This idea argues for the power of trying to be just 1% better every day.  When will you realize the smallest changes in your life can change your life.  Go see the sunrise to get your 1% of UNPOLARIZED LIGHT today. 2. When you know who you are; when your mission is clear and you burn with the inner fire of unbreakable will; no cold can touch your heart; no deluge can dampen your purpose. You know that you are alive.

1. The leptin-melanocortin axis, a cornerstone of mammalian energy balance, traditionally viewed through a biochemical lens as a linear cascade of hormone-receptor interactions, harbors profound quantum photochemistry at its core; one that routinely violates kasha's rule. You should know that the eye is proximal to this pathways embedded in the central retinal pathways. This tells us evolution did something rather unusual to it for some environmental reason.

That reason occured 66 milions yrs ago when an asteroid blocked the sun with particulate matter. It changed the spectrum below on Earth. Life had to react to it. As a result neuropsin was innovated at this time.

Kasha's rule posits that photochemical reactions occur exclusively from the lowest excited singlet state (s₁) after rapid internal conversion from higher states (s₂, s₃), minimizing energy waste. yet, in this axis, anti-kasha effects dominate, where reactions proceed directly from higher excited states (s₂ or s₃), enabling ultrafast (femtosecond-scale) transformations that outpace vibrational relaxation and non-radiative decay.

This violation, far from an anomaly in modern mammals, is was a kinetic triumph, allowing selective control of signaling in the hypothalamus, where leptin binds LepRb receptors to activate pro-opiomelanocortin (pomc) neurons, yielding α-melanocyte-stimulating hormone (α-msh) for melanocortin-4 receptor (mc4r) activation, suppressing appetite while also boosting metabolism. This was needed when the sun spectrum was turned off. If you listened to the recent Huberman/Foisbury pod you'd see these two have zero physics backround to even posit this question, yet we know neuropsin sits in front of the entire leptin melanocortin pathway of ALL MAMMALS.

This made the recovery from the last extinction event speed up rapidly. How would this have helped the thermodynamic arrow of time post KT event? Do not ask Huberman or Fosbury. They remain deeply in the DARK because they still think life is about wavelengths exclusively when it is not. Polarization of light is way more important than wavelngth. These two just have piss running down their leg when you mention it to them. Hence why they are afraid to talk about real quantum biology. Physics > biology as a fundamental science.
2. What would a Fosbury/Huberman answer be to this question? They'd do a literature search in journals they know about it. They's never go outside their silos.

They would do a pod and say that their data review shows results confirm that the leptin-melanocortin axis is a well-understood biochemical pathway for appetite and metabolism regulation, and that Kasha's rule violations occur in specific synthetic chemical systems (like azulene or some organic dyes) under particular laboratory conditions exists but it is not a standard biological process within the hypothalamus because the data THEY reviewed says so.
They'd go on and say............
Therefore, there is no scientific basis in reality to explain how this fictional "quantum photochemistry" would have helped the thermodynamic arrow of time post KT when the sun was blocked.

1. If you want to prevent suicide don't call a phone number. Get people at risk in the sun. The amount of sunshine one gets is a protective therapy against suicide. The link below shows it.
jamanetwork.com/journals/jamap… 2. When your eyes, skin, gut, or lung surface are afflicted by light pollution or nnEMF trauma it induces cell damage in heme-based chromophore proteins that liberate something called CpG Islands from our nuclear DNA/RNA or our mtDNA from the cytochrome heme proteins like cytochrome c oxidase. This is how we make water from metabolism. This was the topic of my Patreon blogs on the eye prism of orexin signaling.

It has also been shown in the literature that RBCs homeostatically bind mtDNA, and RBC-mediated DNA scavenging is essential in mitigating tissue injury after CpG-DNA is liberated from heme-based proteins from destroyed cells.

What kind of disease states should we expect to see cf-mtDNA elevated? Any disease where inflammation is induced by heme protein destruction = blue light hazard, SUICIDE, anxiety, depression, nnEMF, sepsis, trauma, and most mitochondrial and RBC diseases tied to alterations in circadian biology. All neurodegenerative diseases fit this bill too.

patreon.com/posts/quantum-…

IQs have been steadily dropping since the 1970s while the gay lifestyle has increased in incidence and prevalence over the same period.

Concerning, to the smooth brainer until you realize technology’s blue light and nnEMF have been expanding in popular use at the same time.
2. A single night of sleep deprivation increases ghrelin levels and feelings of hunger in normal-weight healthy men
ONE. SINGLE. NIGHT........or 1-5 photons of blue light on your retina. Think about that for a moment.ncbi.nlm.nih.gov/pubmed/18564298

All caused by the technocrats use of polarized light. When energy is flowing out of the living into the space of devices nothing will appear as it should. Percpetion is altered because reality is. Elon as a technocrat does not see his own role in this play.

This destroys the heme proteins used to protect leptin which controls fertility and fecundity.

Here's a narrative woven seamlessly for you to review into our decentralized mitochondrial network theory, the Great Oxygenation Event (GOE), UPE signaling, EMFs, and the evolutionary dance of hormones like cortisol and testosterone. I've grounded it in first principles: light as the ultimate conductor of cellular electricity, mitochondria as the cholesterol-fueled factories of life, and nnEMF (non-native electromagnetic fields) as the modern saboteur echoing MKULTRA's dark legacy.

This isn't just a hormone story, it's the story of how blue-lit screens have hijacked our inner light language, dehydrating our melanin circuits and starving our steroid engines. Remember all horomones are light ferry boats.

Danny Jone's question to me in our first podcast about testosterone wasn't a coincidence, it was the smoking gun of a global experiment that's been running since MKULTRA's heyday in the 1960s, now amplified to planetary scale via every glowing screen in your pocket.

Remember the Great Oxygenation Event (GOE) 2.4 billion years ago? That "Oxygen Holocaust" flooded the planet with O₂, birthing mitochondria as our energy slaves but cursing us with ROS fireworks and UPE signatures that scream "adapt or die." When you use and abuse tech you make cells hypoxic. It simulates the GOE on Earth. You are more like Mars and less like Earth.

Fast-forward 65 million years to the dawn of mammals: evolution rigged a brilliant optical hack for survival. Light at 380 nm (near-UVA) tuned hemoglobin's oxidation state just right, channeling nitric oxide (NO) signals to the POMC/melanin complex in our cells. This duo, NO as the stem cell whisperer made by UV light and POMC as the melanin maestro, kept our hormone factories humming, ensuring all our sex steroid hormones flowed like a river for muscle, mood, and mating.

But here's the twist: that setup was gold under sunlight. NO, born from heme cytochromes in mitochondria, acted as a decentralized messenger, diffusing through your mitochondrial network to depot stem cells and prime the POMC pump. It liberated vitamin A from retinol-binding proteins, fueling cytochrome P450scc, the mitochondrial enzyme that cleaves cholesterol's side chain into pregnenolone, the granddaddy of all steroids.

Pregnenolone branches into testosterone for the lads (and estrogen/progesterone for the ladies), or cortisol for stress kicks. This cholesterol transport inside mitochondria? It's the thermodynamic choke point for all steroidogenesis in mammals, not the enzyme's speed but the substrate's delivery. ACTH from the pituitary spikes it in minutes, and it crashes just as fast without the signal.

Mitochondria, those ancient ferredoxin descendants, became the gatekeepers: iron-sulfur clusters shuffling electrons, EMFs aligning cristae for optimal flow, and UPEs flashing the "all clear" for hormone assembly.

Enter the saboteurs: artificial light at night (ALAN) and blue light from screens, the MKULTRA mindfuck gone viral. Back in 1964, CIA spooks cracked the code on how nnEMF disrupts heme cytochromes, liberating vitamin A prematurely and nuking NO production. NO? Destroyed.

Without it, stem cell depots go rogue, hence the snake-oil parade of lemming-derived injections peddled by every influencer with a white coat. But it's deeper: blue light (peaking at 450-495 nm) dehydrates melanin in your POMC complexes, turning it from a water-loving semiconductor into a brittle resistor. Dehydrated melanin amplifies stray DC currents from your phone's RF microwaves, electrocuting the anterior pituitary and gonads like a bad wiring job. Your jewels in the pocket? Zapped daily, dehydrating cells, spiking NaCl, and spreading electrical chaos where it shouldn't, straight to the mitochondrial cholesterol transporters.

Under ALAN, POMC flips from protector to tyrant. It bosses the cytochrome P450scc reaction, but without 380 nm sunlight to oxidize hemoglobin properly, cholesterol piles up undelivered. Mitochondria starve for substrate, cristae misalign under warped EMFs, and UPE signatures flicker like a dying bulb, low coherence, high noise, per Shannon's rules. Result?

Steroidogenesis grinds to a halt. Males lose testosterone at record rates (down 1% yearly since the '80s, per endocrine data), females watch estrogen and progesterone crater, and cortisol surges unchecked, frying adrenals. All your hormone panels?

Garbage light in, garbage hormones out, light controls this mitochondrial bottleneck MKULTRA mapped and weaponized.

Why screens over paper?

Why Obama and Biden's incandescent bulb bans? It's no accident. Society is easier to control without alpha males. Books under firelight preserved the optical circuit; blue-lit screens short it. The ionosphere's RF blanket dehydrates you globally, echoing the GOE's oxygen flood but with silicon instead of cyanobacteria. DARPA and FDA know: centralized MDs push Big Pharma TRT, but my tribe rebuilds the network—sun-gaze at dawn, ground to earth, ditch the blue devil.

Humanity's young bucks aren't broken; they're optically orphaned. Reclaim the 380 nm key, restore NO's whisper to POMC, flood mitochondria with cholesterol via real light, and watch testosterone roar back. The GOE taught us adaptation; MKULTRA's sequel demands revolution.The implications? This is the Danny Jones podcast on steroids, your low T isn't lifestyle; it's light warfare. Tune your mito network, or stay a lemming.

Retards like @axhoff never did their due diligence. They just post their ignorance because they are arrogant because they never put the PoW into the science. 2. Proof of science? PoW? See the top line.

1. You're only as good as your weakest link.

In decentralized medicine we look at your heteroplasmy ration for each organ.

Here is a sample I hand out to every client after their first private visit to me in El Salvador.

Aging is not one number. Each organ tells its own story about how much polarized and unpolarized light the owner of the organ has allowed. 2. Variation in Heteroplasmy Changes: Wallace enters my clinic exam room

Heteroplasmy (mixed wild-type/mutant mtDNA) disrupts the uniform 30 MV/m field, as mutants impair ETC (e.g., complex I/IV), causing charge mosaics that some see as a bioenergetic "interference" driving disease and evolution.

The main risks related to stereoisomers arise if a supplement contains an incorrect or mixed (racemic) form of a chiral compound:
Different Biological Effects: One stereoisomer may be active and beneficial, while the other may be inactive or even harmful. For example, the body primarily uses L-amino acids, and D-forms are often less bioavailable or utilized differently.
Toxicity: In the pharmaceutical world, the wrong enantiomer has, in some historical cases, shown different toxicity profiles, including teratogenicity or organ-specific harm.

For example:

The thalidomide tragedy of the late 1950s and early 1960s. This historical case points out what I am referring to in the peptide world or amino acid world of supplements. You never hear the food guru or peptide gurus tell you about the history of this risk so here you go.

Thalidomide was sold as a racemic mixture (containing equal parts of two mirror-image molecules, or enantiomers) and marketed as a safe sedative and an effective treatment for morning sickness in pregnant women. The different enantiomers had drastically different effects:

The (R)-enantiomer was the effective sedative with the desired therapeutic effect.

The (S)-enantiomer was a potent teratogen, meaning it caused severe birth defects in developing embryos, particularly affecting limb development (phocomelia), as well as eye, ear, heart, and internal organ development.

An estimated 10,000 to 20,000 infants in 46 countries were affected by these deformities. Many believe as I do these numbers are way under reported.

Crucially, even if the "safe" (R)-enantiomer had been administered alone, it would have been ineffective in preventing the harm because the human body's metabolic processes convert (R)-thalidomide into the toxic (S)-enantiomer, and vice versa, in a process called chiral inversion.

This disaster was a turning point in pharmaceutical regulation, leading to much stricter drug testing protocols and an increased understanding and focus on the importance of stereochemistry in drug development and safety testing. This was never applied to the peptide markets FYI. You have to TRUST that the lab or pharmacy does these tests.

https://x.com/DrJackKruse/status/1992222644561645676

2. More to worry about? Some peptide users in my client have developed amyloid changes. What did I tell them about continued use?

You might create a neurodegenerative disorder in your brain. Why?

Amyloid Beta (Aβ) peptides: In vivo, Aβ peptides, linked to Alzheimer's, can be found with D-amino acids (specifically Asp and Ser residues), indicating that a natural inversion process occurs, which affects their aggregation properties. This is an example of chiral inversion. This kind of freaked them out. When they questioned the lab/pharmacy and longevity docs who gave them this stuff communication completely shut down.

Decentralized medicine aims to educate not induce fear.

Today's PSA 2. The follow up idea is below. If it is isnt science it is PROPAGANDA

Tissue polarization by artificial light turn the matrix of mitochondria into a deuterium-gated racemization factory, turning mitochondrial proteins into mirror-image versions that:

a. reverse CISS spin filtering,
b. invert local PV asymmetry,
c. emit optically “backwards” UPEs that neighboring healthy cells can no longer read correctly,
d. and render affected cells invisible to immune surveillance by NK cells (D-peptides are non-self to TCRs that evolved under L-only rules).

https://x.com/DrJackKruse/status/1991999231373230464

2. COVID was more than a virus—it was a Parity Violation inversion, hijacking the iron at the center of life’s light engines. By disrupting heme, it dimmed the internal sun of billions. Homochirality allows for the precise folding and functionality of complex structures like mitochondrial matrix, proteins and RNA/DNA, which is essential for the high energy efficiency of aerobic life.
A "global change in homochirality" in a body was changed by the spike protein and was indeed catastrophic to the compliant, on an oxygen-dependent food web because ALL of that machinery of life relies entirely on this specific asymmetry.

1. Centralized medicine 101 here:  nytimes.com/2007/11/25/mag… 2. Hi Jack,

Wondering if you'd be able to break down what happened after I took Venlafaxine (Effexor) a few years ago and if there's any specific things needed to be done to hopefully repair any damage.

After what I believe was a spontaneous CSF leak that happened one night and started all my chronic issues I was diagnosed with vestibular migraine around 3 months later.

Venlafaxine 75mg was indicated for this so I was on it for around 12 months (give or take the 3 months wean I did).

Within 3 weeks my emotions went numb, I lost my libido, erections and ability to pretty much feel love or any strong emotion. There was a very definite and obvious "change" but I believe I still had the ability to focus and enjoy hobbies etc.

After deciding to taper off, I would get brain zaps and all the other jazz that comes with it. After fully tapering, I was then introduced to anhedonia. Unable to feel or enjoy anything, unable to focus on anything for too long without getting the irritable and feeling like I need to do something else etc. Essentially feel there's been a permanent change since starting this.

This has improved slightly but not even close to where I'd like to be. Add all the daily brain fog, memory lapses etc and my brain is running on empty.

Does this need anything specific additional to the core light, water & magnetism?

Listening to this months webinar you mentioned accutane extending recovery from 6 months up to 5 years. This prompted me to ask this question and about my accutane use in the future as this is a huge jump in recovery time and shows how powerful these drugs are.

Thanks,
Ja$%^

1. I just gave a talk to a group of medical students..........Here was my only slide. 2. Here was the substance of the talk.

The talk was a sobering discussion for me, yet it empowered my reflection on navigating a world where societal dogma often clashes with truth.

I explored how civilization rewards comfortable lies while penalizing painful truths.

What don't sunglass and eye glass manufacturer's know? Polarized light and lenses are used as a tool to detect and measure the tiny effects of Parity Violation in atoms and molecules, where the weak force causes a slight "handedness" in physical systems that are otherwise mirror-symmetric.

The core link is that the weak force's violation of parity symmetry leads to a mixing of atomic or molecular states that should, under normal circumstances (governed by the parity-conserving electromagnetic and strong forces), have a definite, opposite parity. This mixing is extremely small but results in two primary observable effects involving polarized light. It affects water networks and all proteins that interact with the polarized light.

Note: all artificial sources of light are POLARIZED.

When linearly polarized light passes through an atomic vapor or a chiral medium like the human eye, its plane of polarization rotates slightly. The amount of rotation is related to the degree of parity violation in the atoms distal to it.

Materials exposed to the weak interaction can show a minuscule difference in how they absorb left-handed versus right-handed circularly polarized light. Why is this a big deal in my human patients?

Stellar masses are designed to use you as their lens. This is why DNA codes only for semiconductive proteins that all have absorption and emission spectra.

Parity vioation in your tissues explain life's universal preference for L-amino acids and D-sugars, a puzzle since Pasteur's 1848 discovery of molecular chirality. when you wear lenses in front of your eyes or bath in light man makes you just broke a fundamental law of Nature and it always leads to DISEASE your doctors are impotent to repair.

https://x.com/DrJackKruse/status/1930629376795627528

2. Just how big a deal is this? This is why the meat head carnivores and the longevity doctors need to be ignored. It could lead you to a nasty disease.

Consense is pseudoscientific. Science is about asking difficult questions and having sloppy answers and results.

Why did the Zionist post Lansky opt to control PEER science via PERGAMON Press and others? Control of the narrative. This is why Eric Weinstein found it so unusual that Epstein was linked to funding his math and physics depts at MIT.

Epstein funded many of the cypherpunks for the same reason. Post Lansky and into the the Chaum and Sassaman epoch programable money went from closed source to open source. The accountant for Murder Inc lost the allodial title to what would become Bitcoin back then. So Epstein was hired by the Zionists to check on the state of affairs to see how he could main control over it without owning it. Lansky 101.

Many of the early cypherpunks were also transhumanists. Many of them became OG Bitcoiners. And Epstein funded them all for the same reason Lansky followed J Edgar Hoover, to use them and control them. He wanted to see how good the filters were being used in PEER review under the Maxwell clan in filtering centralized science from high signal decentralized science for control. This system was the earlier system to Google's ability to do the same thing view SEO search. Now this is used by Palantir.

Cypherpunks and US Intelligence: WikiLeaks, EFF and TOR Many top cypherpunk cryptopgraphers (some already mentioned earlier in this thread) are linked to US intelligence. Similarly, many early Bitcoin and crypto pioneers have ties to intelligence agencies, adding to the likelihood that Bitcoin originated from the US NSA or CIA (bullshit), with the help of cypherpunk assets under the guise of “anti-government” libertarianism through decentralization for a more fair and completely private monetary network.

This is simply a farce cover story and there is most likely “backdoor” access from the US government intelligence (maybe other government inteligence as well such as Israel’s 8200 Unit). Lansky money was behind Chaum when it was closed. Sassman opened sourced it and they lost control of it. This is similar to the PROMIS software of the 1980’s that was sold as “secure” when the NSA had access (as well as foreign intelligence agencies) nearly the entire time it was use and sold around the world.

Several of the cypherpunk and libertarian assets tied to Bitcoin are also “whistle-blowers” against the US government. This is another cover for the storyline, meaning they are likely playing roles to give the illusion of brave heroes going against the machine or “big brother”. These whistle-blowers include Julian Assange, Chelsea Manning and Edward Snowden.

Edward Snowden, famously leaked thousands of classified documents including the global surveillence program, inlcuding PRISM, was a former contractor for Booz Allen Hamilton. CALLEY MEANS WORKED for Booz Allen as I exposed on Danny Jones.

Booz Allen Hamilton, a major U.S. government contractor, has deep ties to the CIA and broader intelligence community, employing over 1,000 former intelligence officers and securing $1.3 billion in intelligence contracts annually as of 2013. Snowden held positions in both the CIA and NSA. He is assocaited (or was) with several relevant cypherpunks, including Moxie Marlinspike, Jacob Appelbaum, Runa Sandvik and several others.

Snowden recieved help from Julain Assange when Sarah Harrison, sent by Julian Assange, helped Snowden secure asylum in Russia, accompanied him on his flight, and stayed with him for 39 days in Moscow’s Sheremetyevo Airport, later ensuring his safety in Russia after his massive leaks were made public.

Mentioned earlier in the thread, Julian Assange was a member of the Extropy Institute. Chelsea Manning, a former U.S. Army intelligence analyst, leaked over 700,000 classified documents to WikiLeaks in 2010. He then orchestrated the release of U.S. military and diplomatic leaks, including the Iraq and Afghanistan war logs, sparking global controversy.

Coincidentally, Chelsea manning (a transgender male to female) once dated Elon Musk’s ex “Grimes” (Claire Boucher) [likely also a transgender male to female]. Chelsea Manning was also close with cypherpunks like Isis Lovecruft and Yan Zhu. Yan Zhu was an intelligence analyst for the US DoD, as well as a ‘Hacker Comununity Organizer’ for Noisebridge, a “hackerspace” noteable in the cypherpunk community. Yan Zhu was also a member of the Electronic Frontier Foundation.

So what was Epstein doing monitoring Hal Finney, Adam Back, Eric Weinstein, and Peter Attia? He was making sure they found nothing out in science that mattered much at all to his bosses in Banking and BigHarma. He was the feedback loop to understanding how they could keep order and control.

The Electronic Frontier Foundation (EFF) is a nonprofit organization dedicated to defending digital privacy, free speech, and innovation through litigation, policy advocacy, and technology development. Noteable members of the EFF include: Hal Finney, Jacob Appelbaum, Yan Zhu and Esther Dyson. Esther Dyson worked closley with many transhumanist and cypherpunks.

She also worked with Barney Pell of Singularity and Bing! (Microsoft) as well as received funding from Jeffrey Epstein for her research on transhuman and longevity science. She worked at Space Adventures with XPRIZE founder Peter Diamandis. Diamandis also is a member of Singularity with Barney Pell, Ray Kurzweil, David Bray and Cathie Wood.

Cathie Wood funds many Elon companies and Peter Thiel’s Palantir. Todd Huffman worked with the US DoDlike Yan Zhu, specializing in intelligence analysis. They also are both members of Noisebridge mentioned before, the “hackerspace” community event for cypherpunks. He also worked extensively with DARPA, helping found and operate the TOR Project. The Tor Project, founded in 2006 as a nonprofit, develops Tor, a free, open-source network that enables anonymous communication by routing internet traffic through multiple volunteer-operated servers to conceal users’ identities and locations.

It protects against surveillance, censorship, and tracking, and is widely used by activists, journalists, and privacy advocates. This is a very similar “project” to Bitcoin in terms of privacy, operations and libertarianism. It was funded by the US goverment and developed at the US Naval Research Laboratory. With Sassaman, they lost the control of Bitcoin allodial title and now as I just discussed with @BTCsessions team of Nathan and Paul today they are going to use the State surveillance to enforce control.

Most people have no idea why Back, Finney, Weinstein and Attia were on Epstein's radar, but I do. Keep people sick and dumb is what tyrant do to maintain order in their fiat kingdoms. cbsnews.com/news/jeffrey-e…
2.

https://x.com/DrJackKruse/status/1990189827245920567

Why Two People Can Eat the Same Meal And Have Completely Different Biological Outcomes

We’ve all seen it:
Two people follow the same diet.
Same calories. Same macros. Same discipline.
One thrives. The other struggles.

For years, we blamed willpower, hormones, or “body type.”
But the truth is far more interesting and far more hopeful.

What most people forget is their light environment varies and the amount of light on their skin, eyes, and abdomen vary and that light changes prokaryote biology. Since mitochondria used to be a prokaryote it changes them to to alter UPE signaling. It is this light that changes the microbiome in you.

Inside every one of us lives a huge microbial ecosystem that is designed to act like soil around a tree. That colony of microbes then alters the type of bacteria by the light mitochondria release and that sculpts how we metabolize, respond, and recover.

It was never just the food that did it. Jeff Leach proved that in 2017.
It’s how your microbiome interprets the electromagnetic bar code embedded by the sun in your food.

Here’s what emerging research is revealing:

Some individuals harbor more Bifidobacterium longum and Faecalibacterium prausnitzii, which are bacteria shown to convert dietary fibres into short-chain fatty acids (SCFAs), improving gut-barrier integrity and lowering systemic inflammation (Zheng et al., 2020; Guo et al., 2021).

Oxygen is a toxin to prokaryotes so when you live within nnEMF light of any kind the sphincters in the gut to let oxygen roam free. This simplfies and the gut and leads to alien UPE signaling which causes disease.

Others show a higher Prevotella-to-Bacteroides ratio a microbial signature that can predict post-meal glucose spikes more accurately than the glycaemic index itself (Zeevi et al., 2015; Kovatcheva-Datchary et al., 2015). Of course the amount of sunlight is a critical variable these studies missed. We already know from other studies that sunlight reduces blood glucose by 30%

And in women with PCOS, increasing levels of Akkermansia muciniphila correlate with stronger gut-barrier function, lower endotoxin leakage, and improved insulin sensitivity (Depommier et al., 2019; Liu et al., 2023). Solar power increases gut barrier strength (Reverse Frey Effect while lowering endotoxin loads and improving insulin because it is a solar hormone.

This isn’t old-school nutrition.
This is quantum biology explaining the nuance food gurus miss.

We are entering the era of precision nutrition, where we move beyond calories and start decoding microbial fingerprints.

Where 16S rRNA sequencing, metagenomics, and metabolomics help us design diets that work with the gut ecosystem rather than against it.

The future of nutrition isn’t about restriction.
It’s about interpretation.
Intrepration of the UPEs the microbiome makes is key.

Same meal.
Different microbiome.
Different biology.
Different outcome.
UPEs are the kinetic force carrier of this change.
Light is how we sculpt our outcomes.

Stop Feeding Your Gut Bacteria, Start Feeding Your Gut Environment

Humans don’t have a bacteria problem in their guts; you have an ecosystem problem related to the light you imbibe that changes the prokaryotes in your gut.
Most probiotics fail because we’re feeding the wrong thing. The microbiome needs light from the sun.

What most need to learn now is how we reshape the approach to these topics to sculpt humans
• metabolic health
• mental health
• PCOS and women’s health
• autoimmune disorders
• and even biological ageing

The gut isn’t just a passenger.
It’s a conductor for light.

And it’s time we started listening to this reality.


2. Biophoton Emission in the Colon and My Decentralized Thesis

My thesis posits that bacteria in more hypoxic environments (like the colon) emit more light, particularly in the ultraweak UV range, and that this light interacts with the gut wall, potentially explaining the high VDR expression in the gut. The colon, with its dense microbial population (10¹¹ bacteria/mL, as per my slide), is a strictly anaerobic environment where bacteria like Bifidobacteria and Bacteroides ferment complex carbohydrates. I previously estimated their biophoton emissions to peak in the visible range (500–600 nm) due to fermentation-based metabolism producing fewer reactive oxygen species (ROS) compared to oxidative metabolism. However, if we assume a shift toward the near-UV range (300–400 nm) in the colon, perhaps due to specific light stress responses, metabolic byproducts, or unique redox reactions in anaerobes, this would have distinct implications for colonic processes. Blue light and nnEMF can do this.