LightOverPrism

A banana in January in New York floods your mitochondria with deuterium. Your body has no tools to handle it. Dr. Laszlo Boros — former professor of pediatrics at the UCLA School of Medicine & pioneer of deutonomics — explains why seasonal & local eating isn't just a dietary preference. It's a fundamental requirement for mitochondrial function. Three independent mechanisms explain why. 1) Sunlight and photon pressure: Tropical fruits are naturally high in deuterium — the heavy isotope of hydrogen that causes ATP synthase nanomotors inside your mitochondria to stutter and break. In equatorial regions, high-intensity red and infrared sunlight penetrates the body and decreases the viscosity of water inside mitochondria — allowing the nanomotors to keep spinning despite the deuterium load. Eat that same banana in a dark New York winter — without the corresponding sunlight — and your mitochondria receive the heavy fuel without the light needed to process it. The nanomotors stall. 2) Microbiome desynchronization: Your gut microbiome is your primary deuterium filter. Here's the mechanism most people miss: Bacteria actively collect deuterium to fuel their own division. They run their nanomotors in reverse — pumping clean protons out while trapping heavy deuterons inside their cells. As they ferment your food, they strip out the deuterium and release deuterium-depleted metabolites — short-chain fatty acids and ketone bodies — back into your gut for clean energy production. The trapped deuterium gets excreted in your stool. But this filtering mechanism only works when your microbiome is adapted to the food you're eating. Bacteria are highly specialized. They only efficiently metabolize a narrow range of substrates. When you eat a consistent local diet — your microbiome develops a stable tailored population that knows exactly how to extract deuterium from those specific local foods. When you introduce an imported tropical fruit in winter — your gut bacteria are caught off guard. They haven't adapted to this foreign substrate. They can't ferment it efficiently. They can't trap the deuterium fast enough. It slips past the gut's mucosal barrier directly into your circulation — and into your mitochondria. 3) Nanomotor stutter and metabolic crowding: Inside your mitochondria are ATP synthase nanomotors — spinning at up to ~9,000 rotations per minute to pump protons and produce energy. A deuteron is twice as large and twice as heavy as a normal proton. When it enters these fast-spinning motors — it acts like a medicine ball thrown into a precision engine. It becomes stuck. The nanomotors stutter and break. The consequence is metabolic crowding. With the motors destroyed, protons can no longer return to the mitochondrial matrix to mix with oxygen and form metabolic water. Complete biological combustion stops. Just like an engine choked with fuel but lacking a working exhaust — your mitochondria can no longer fully burn incoming carbohydrates, fats, and proteins into their natural end products of carbon dioxide and water. The unburned fuel backs up and piles up inside your cells. Your body stores it as visceral fat, excessive glycogen, or abnormal proteins. This is metabolic crowding. And it is the biochemical root of obesity, diabetes, and cancer. Boros: "When you walk into a department store and you see those shiny apples and watermelons from wherever they're from — it's really not your food. First of all, it doesn't grow there, especially not in that season. And when you eat it, you don't have the light exposure, the oxygen partial pressure, and you name it." Eating locally and seasonally isn't a wellness trend. It's what your mitochondria were built for.

The sun is Nature's original doctor, and your mitochondria are the original pharmacy, but the hospital you get well in is the magnetic dyanamo you draw your power from.   This quote is from my new book, "Health and Wealth Are The Same Fight." New blog out that continues the story I unleashed today on "X" about the magnetic excursion you are experiencing now.  https://t.co/PgiImpFgwe Be prepared to be more stunned about how the Nubians survived their excursion.

If they understood what the telomere inside of the bulk of Chromosome was doing they would know aging is tied to the ratio of D+ to H+ in a tissue. D+ in the blood does not age you because RBC have no mitochondria. Everyother tissue has mitochondria and when it gets deuterated it ages and NAD+ becapmes NADD+ = KIE destroys the costly in time Eukaryotic Langrangian When time symmetry is lost atomic mass is added to the base chain of DNA and you get sick first and die sooner = time loss is aging.

This study reinforces why Kruse consistently emphasizes: • Deuterium depletion (DDW) • Structured water / dielectric constant restoration (EZ water) • nnEMF avoidance and coherent light environments • The impact of Earth’s declining magnetic field on mitochondrial function These are all upstream factors that affect local tissue coherence and grace buffer width — far more aligned with the Ledger than chasing blood NAD+ levels. Bottom Line Dr. Kruse is correct — this study is another meaningful blow to simplistic, blood-marker-driven longevity marketing. It highlights how much of the commercial space has been measuring the wrong thing and selling solutions based on flawed assumptions.

The newly published, peer-reviewed study from Nature Metabolism (May 2026)represents a major shift in longevity science and deals a heavy blow to the commercial narratives popularized by David Sinclair. By analyzing over 1,100 human samples using state-of-the-art mass spectrometry, researchers confirmed that whole-blood NAD+ levels remain completely stable across the human lifespan, directly dismantling the baseline assumption that aging causes a systemic, measurable drop in blood NAD+. This study exposes a critical flaw in how anti-aging metrics have been marketed to the public. For years, the commercial longevity industry has sold blood tests and supplements on the premise that what is measured in a blood draw reflects the biological health of peripheral tissues. 1. The Breakdown of the Longevity Proxy The Nature Metabolism paper outlines exactly why using blood as a proxy for systemic aging is a major scientific misdirection: Compartmental Isolation: Unlike glucose, which equilibrates across the entire body to supply energy, NAD+ is synthesized locally within individual tissues. Blood as a Poor Surrogate: Whole-blood NAD+ primarily reflects the internal metabolic activity of circulating cells (erythrocytes and leukocytes). It does not act as a window into the state of skeletal muscle, hepatocytes, or cardiac tissue, which are the primary sites of age-related decline. The Failure of Lifestyle Benchmarks: If NAD+ were a true dynamic biomarker of health and vitality, lifestyle changes that improve mitochondrial health should shift its baseline. Yet, six months of intense resistance training, strict adherence to a Mediterranean diet, or being an elite endurance athlete showed zero change in blood NAD+ levels compared to sedentary individuals. 2. The Unraveling of Sinclair’s Longevity Narrative is bad news for his supporters . This study adds to the growing scientific pushback surrounding David Sinclair's research. Sinclair's career has faced intense scrutiny from peers within the Academy for Health and Lifespan Research, leading to his high-profile resignation following backlash over exaggerated claims regarding "age reversal" supplements in dogs and gene therapy in primates. For influencers incentive always dictate their support. Savages should not forget this. The core issue is that Sinclair’s promotional platforms presented preclinical rodent data as human fact. While early mouse models showed tissue-specific depletion, independent labs have consistently struggled to replicate Sinclair's broader translation to humans. The Nature Metabolism study demonstrates that the trillion-dollar longevity market has been measuring the wrong compartment and inferring benefits that lack clinical backing Do not forget what the influencer said. When you get paid for the bad adivce the truth usually suffers a great deal. 3. Shift from "Nutrient Deficiency" to "Pharmacological Push" This discovery reframes how NAD+ precursors, such as Nicotinamide Riboside (NR) and Nicotinamide Mononucleotide (MNM), must be viewed. No Deficiency to Correct: Supplementation does increase blood NAD+ by roughly 40%, but it is not "restoring" a missing molecule like vitamin C for scurvy. A Forced Pharmacological Action: Because there is no natural systemic deficiency in healthy blood, taking these supplements is actually a pharmacological push. It forces the overexpression of NAD+-dependent enzymes (like sirtuins or PARPs) independent of baseline health. This completely changes the risk, safety, and dosage dynamics for anyone in their fourth or fifth decades of life. Forcing a continuous chemical surplus in a system that naturally maintains tight homeostatic regulation carries completely different long-term biological consequences than correcting a natural decline.

New Podcast: https://t.co/AcbIygLCyd One point needs to be more clear because of what you think you just HEARD in this podcast: Your exterior tan tells you about your exterior........but not the interior dielectric pressures. That might related to the ability to think well and properly via homocysteine levels. Vitamin D levels, hormone panels, TMAO levels, White matter changes on MRI, or slow flow on a thermogram. The interior tan (melanin) is more important to humans than the exterior open because it links to COGNITION and wisdom. Why? This is the "Internal/External Phase-Shift." I’ve hit the most profound clinical distinction in the entire decentralized framework: Melanin in the skin is the "Faraday Shield," but Neuromelanin in the brain is the "Quantum Processor." If your exterior tan is deep but your interior is "Maillard-browned," you are a high-performance shell with a stalled engine. The interior tan is the measure of your 160THz coherence in the Obex, the Substantia Nigra, and the Locus Coeruleus. 1. The "Frosted Lens" of the Interior You can have a perfect exterior tan (UV-Melanin rectification on the crust) but still suffer from Isotopic Stagnation in the brain's "Water Table."See Los Angeles as the classic Kruse example.........good tans and dumbassery walking on Rodeo drive. The Signatures: High Homocysteine and TMAO are the biochemical "silt" markers. They tell you that the Right Vagus and the 2L Bicarb Flush are failing to clear the Deuterium. The MRI/Thermogram Proof: White matter changes and "slow flow" on a thermogram are the macroscopic views of Increased Viscosity. The "internal pipes" are filled with "ketchup" (heavy water), slowing the Transition Probability of the DC current. 2. Cognition, Wisdom, and the 160THz Signal: MKULTRA Consciousness is a function of the Internal Dielectric Pressure. The Processor: Wisdom requires high-speed Proton Tunneling across the neural semiconductor. If the internal dielectric constant is dropping from 160 toward 78, the "Phase-Lock" to the Universal Stator is lost. The Haze: You might look "healthy" on the outside, but if your NAD+/NADH ratio is "heavy" (deuterated), your cognitive "OS" is downgraded to DOS. You lose the ability to "process" complexity and fall into the "Survival/Dopamine" mode. 3. The "Melanin-POMC" Disconnect As Mat noted with his N=1 in this thread, the MITF-AMPAR pathway can be "fooled" by local variables. Exterior Tan: Tells you the skin is successfully "quenching" the environmental noise. Interior Tan: Tells you the Heme-Melanin axis is successfully producing DDW to cool the IMM. The Conflict: If you are grounded but still drinking 155 ppm water in a high-declination zone, your skin will tan, but your Internal Lattice will still "Lattice-Lock" because the D-Speed Bumps are entering through the gut/water-table = most of humanity. 4. The "Z-Axis" of Wisdom Wisdom is the Asymptotic Optimality of the brain's quantum ensemble. It requires the 7.2-second "Quiet Time" between isotopic collisions to allow for the Intersystem Crossing (ISC) into the Triplet state. If the interior is "noisy" (High UPE/Low Dielectric), the "Wisdom signal" is lost in the Maillard-Orange heat. You are "Zapped" on the inside while being "Golden" on the outside. 5. The Synthesis: The True De-Frag The goal of the 92.5 ppm DDW / 3% NaCl / UV protocol is to "Tan the Interior." It lowers the Internal Viscosity so the 160THz signal can reach the Pineal and Pituitary (The Empty Sella check). It clears the Obex so the "Cognitive Highway" is frictionless so you can avoid things like ALS or oxalate damage or stiff man syndrome Jordan Peterson diseases. My Conclusion: An exterior tan is a "badge of effort," but a clear Internal Dielectric Pressure is the "State of Grace." It is the difference between a "Human Billiard Ball" and a "Topologically Protected Quantum Sovereign." The "Z-Axis" doesn't just keep you alive; it allows you to see the "Universal Stator" clearly. The Y-AXIS is the Windex on your glass eyes which wipes deuteration away.

The focus on the "bell curve" is the foundational trap of modern biochemistry. It assumes human biology is a static, averaged soup of chemical inputs and outputs. By contrast, biophysics views the organism as a dynamic, non-linear, liquid-crystalline semiconductor. In this framework, "outliers" are not statistical errors to be medicated back into a standard distribution; they are the logical result of an individual's unique quantum interface with a shifting environment. Know this: Roger Williams’ Biochemical Individuality mathematically proved that if you measure enough variables, the "normal" person ceases to exist. Let that sink in. Biochemistry looks at the pieces of the car; biophysics looks at the electricity running the engine. When medicine focuses strictly on chemical biomarkers (like forcing a statistical outlier's cholesterol down via a statin), it treats symptoms while completely ignoring the underlying physics: The Isolated Fragment: Biochemistry measures a static number in the blood at a single point in time, completely isolated from the environment. Nick loves to do this in his tweets. He remains deeply ignorant of how a cell really operates. The Integrated Reality: Biophysics recognizes that your unique biomarker profile is a real-time reflection of how efficiently your Inner Mitochondrial Membrane (IMM) is trapping electrons and pumping protons. Your "outlier" status is often your body's intelligent, non-linear adjustment to preserve its overall electrical voltage.

Dark mode prevents myopia (nearsightedness). Dr. Alexander Wunsch, German physician studying the effects of light on health for 30+ years: "Whenever the opportunity arises to read text white on black, we should do so." Here's the mechanism: Your retina has two cell systems — ON cells and OFF cells. Black letters on white background activate the OFF cell system. Chronic activation of the OFF cell system promotes the development of myopia. Dark mode — white text on black background — activates the ON cell system instead. This is the preventive mechanism. There is also a significant difference in total light load: > Standard display (white background, black text): 95% of screen light is emitted to display the page. Only 5% is the actual text. > Dark mode (black background, white text): only 5% of total light is needed to convey the same information. Less light from the screen. The correct cell system is activated. Lower myopia risk. The first computer screens were dark mode by default — black background, green or amber text. That was optimal. The shift to white backgrounds was aesthetic, not biological. University of Tübingen, 2018 — researchers developed a mathematical model analyzing image content for myopia risk potential. Their finding? Natural outdoor scenes have a neutral effect on the eye. Conventional text on white background promotes myopia development. Dark mode presentation does not. They then tested this in subjects. Black letters on white background produced measurable changes in the eye that promote myopia. In Europe, half of all students are already nearsighted. Myopia is the most common visual impairment among young people. The more a child reads — the higher the risk. The mechanisms are not yet fully understood in all details. But the consequences are clear. Wunsch: "Dark mode is recommended wherever it does not impair the workflow during screen work." "In the evening and at night, this should be the mandatory setting in order to keep the disruption of the internal clock and the possible damage to the retina as low as possible." Wunsch's advice to parents: "If children discover the joy of reading and develop into bookworms, it is certainly a good investment to provide them with an e-book reader that enables text display on a dark background." The original screen setting was black background. We changed it for aesthetics. The biology didn't change with it.