Man has lost his humility with progress. Humility is simply nature’s disposition that prepares our minds for living on intuition. Nature's disruption is what human life should rely upon. This process is controlled by sunlight and should be uncontrolled by man-made light. Man-created algorithms to try to fix the problems they cause. The AI algorithms made things worse for the public's health. The algorithms served the centralized institutions' profit purpose. Many do not realize these algorithms are a proxy for manufactured light. Manmade light has usurped this process and has led our species down a dark alley of disease. These diseases confound centralized institutions. This has made our brain preoccupied with technological progress, which is now leading to biological disruption. This is the real reason everyone needs to run towards decentralized systems. Nature is that decentralized system.

My solar strategy is simple. It is to acquire information about the tactics of 'time' my cells need to win. Without the bounty of solar tactics, the road to Optimal becomes brutal. This is the slowest route to victory for our cells. Tactics without strategy are the noise before the mitochondrial illness. Man must live according to how nature built him to operate in her framework. Mythology didn't cease to exist and be useful to pagans when we gained digital watch technology. Technology has changed humanity and redirected us to the road of destruction. The fog of information from technology has blinded us from our natural wisdom.
linkedin.com/pulse/your-mic…

2. All things in nature operate by the interactions between wavelength spectrums.
Humans decode these sunlight-based spectrums with their senses. (aka Human 1.0)

-Algorithms are machine language, 1s and 0s, and essentially void of any connection to full spectrum nature.

They are the weapon of the profiteers of centralization and control whether it be your medical record, your purchase history, or your containment in a “15 Minute City.”

Imo, not only are these machine language algos destructive at the individual level, but they are an attack on humanity.

I want no part of any centralization and consolidation into a totalitarian controlled Human 2.0 centralized existence which relies on machine language and not sunlight.

Many cultures in human history have known the importance of the Sun. The idiots that put themselves in charge of this current time/space are talking about blocking the sun, again this week.

That’s all you need to know right there with that little factoid.

4. Light exposure—say, sunlight or specific wavelengths—impacts circadian rhythms via the suprachiasmatic nucleus in the brain, which regulates hormones like melatonin and cortisol. These hormones influence metabolism, including fat tissue activity where FIAF is expressed. Fasting, which boosts FIAF, is also tied to light cycles—think of how daylight affects feeding patterns. If biophotons reflect or amplify these light-driven processes at a cellular level, they might indirectly tweak FIAF production by signaling energy states or oxidative stress in cells.

My decentralized ideas have always been spot-on that this topic doesn’t need a scientist to spell it out in a paper—absorption/emission spectra are measurable, and biophoton emissions are detectable. The gap isn’t in the physics; it’s in tying the specific wavelengths of biophotons (which vary by cell type and state) to FIAF’s exact optical profile in vivo. Still, if gut cells emit biophotons in, say, the 300-400 nm range, and FIAF absorbs there, is the optical photonics interaction a real—study or not? It’s like saying water absorbs infrared; we don’t need a new experiment to prove it gets hot under sunlight. We do not.

5. Fritz-Albert Popp’s work on biophotons does indeed highlight a massive difference: bacteria, as prokaryotes, emit biophotons at rates orders of magnitude higher—up to 5,000 times more—than eukaryotic cells like ours. That flips the script on the gut’s light environment, and Peat should have considered this during my discussion with him and caught how that amplifies the signal I'm driving at.

Popp’s research showed bacteria churn out biophotons—think UV to near-infrared, peaking around 200-800 nm—through the metabolic hustle of mtDNA, mainly oxidative reactions. In the gut, with trillions of bacteria in the microbiome, that’s not just background noise; it’s a flood of light. The gut-associated lymphoid tissue (GALT), sitting right there with immune cells and epithelial barriers, is bathed in this bacterial biophoton output. If we’re talking 5,000 times the intensity of human cell emissions, the gut’s lightscape is dominated by prokaryotic chatter, not our own cells.

Peat would have been stunned by the paper below but he refused to listen to Uncle Jack.

6. Now, FIAF—produced by gut and fat tissue—has its optical fingerprint, absorbing light (say, UV around 280 nm from its aromatic amino acids). This bacterial biophoton barrage could hit FIAF directly, exciting its molecular structure far more than eukaryotic emissions ever could. Picture it: a constant, intense light signal tweaking FIAF’s conformation or activity, ramping up its inhibition of lipoprotein lipase. More FIAF action means less fat storage, shifting the gut’s nutrient pool—less lipids for bacteria to munch on. This could steer microbiome diversity hard, favoring lean-adapted species (like Akkermansia or Bacteroidetes) over fat-thriving ones (Firmicutes), just as you see in fasting states where FIAF spikes.

But it’s not just FIAF. That bacterial light flood could signal across the gut-GALT axis, influencing epithelial cells, immune responses, and even microbial gene expression. This light signal controls T regulator cells to program into other T cells like NK Killer cells and TOLL receptors.  If this light signal is off, many diseases we have no answer for in centralized science are possible, like cancer, autoimmune conditions, and neurological issues related to the brain-gut axis.  This would affect the electrical signals that maintain all the barriers in our organ system, which Michael Levin has discussed in his work.

Bacteria themselves “read” each other’s biophotons—using their chromophores Popp suggested coherence in these emissions could coordinate behavior. In the gut, this might mean quorum sensing on steroids (check my podcast out I did with Kriven Govender on the gut years ago warning quorum sensing is the ticket), with light shaping which species dominate based on who thrives under the energy conditions FIAF helps set = Roeland Van Wick book.

7. Light’s role here is hard to fathom for centralized science but it is REALITY: if biophotons from bacteria (UV to near-IR, coherent per Popp) hit photoreceptors or chromophores in gut cells and their mitochondria, they could trigger signaling cascades—say, via calcium fluxes or redox shifts—that reprogram T-regs. Studies already show light modulates immunity (e.g., UV affecting skin T-regs), so in the gut, this bacterial glow could be the conductor, tuning NK cell aggression or TLR sensitivity.

If that light signal’s off—too weak, incoherent, or drowned out by modern disruptions like artificial light or poor circadian cues—chaos creeps in. This alteration of the fidelity of the signal is where chronic diseases begin. It is not from food. This is why MAHA is wrong and why putting Calley and Casey Means on team Kenedy was unwise. @SecKennedy

FIAF might falter, fat metabolism skews, and the microbiome shifts toward pro-inflammatory species (more Firmicutes, less Akkermansia). But beyond that, misfired biophotons could scramble T-reg programming, letting autoimmune conditions (e.g., Crohn’s) or cancer (unchecked cell growth) take root. The brain-gut axis fits too: vagus nerve signaling, which Levin’s work on bioelectricity touches, relies on gut barrier integrity. Levin’s shown organs use electric gradients to maintain form—disrupt that with a broken light signal, and barriers (gut, blood-brain) leak, sparking neurological havoc like Parkinson’s or depression.

8. Peat missed the immune and bioelectric scope earlier—at your peril. His OJ advice is deadly when you understand these ideas.  This light-driven model explains diseases centralized science fumbles: cancer from deregulated cell signals, autoimmunity from immune misreads, and neurological decay from gut-brain disconnects. Levin’s bioelectricity ties it together because electricity precedes chemistry in quantum cells: if biophotons shape membrane potentials across barriers, a glitchy signal could collapse the whole system.

Bacterial biophotons—UV to near-IR, coherent as Popp demonstrated—aren’t just background chatter; they’re a high-fidelity broadcast hitting photoreceptors and chromophores in gut cells and their mitochondria. Think opsins or flavins in cell membranes or cytochrome c oxidase in mitochondria, absorbing these wavelengths (say, 300-800 nm).

When the signal’s crisp, it triggers precise cascades—mitochondrial ROS spikes, calcium waves, or gene switches like NRF2 or PPARs—keeping the gut-GALT axis humming. FIAF gets tuned, T-regs stay balanced, and the microbiome aligns with lean, anti-inflammatory species. It’s a symphony of light, not a food-driven plod.

But when that signal degrades—too weak from a gut stripped of bacterial diversity, incoherent from chaotic emissions, or drowned by artificial light’s 24/7 blue glare (think LEDs peaking at 450 nm)—the system unravels. Mitochondria misfire, altering their biophoton emission, missing their light cues; ROS goes haywire, not hormetic.

T-regs skew into overdrive or apathy, TLRs overreact, and barriers (gut, brain) leak like sieves. This isn’t a downstream effect of diet; it’s the upstream signal breaking. Chronic diseases—cancer, autoimmunity, neurodegeneration—don’t start in the kitchen, but in this light, fidelity collapses. Food might nudge the microbiome, but the biophoton distortion, amplified by modern life’s decoupling from natural light cycles, lights the fuse.

Centralized science stumbles here because it’s obsessed with nutrients, not photons.

9. Centralized science stumbles here because it’s obsessed with nutrients, not photons. Popp saw it and taught me to see it: coherence matters more than intensity. A gut awash in bacterial light should sing; disrupt that with screen glare or sterile living, and you get discord—disease. Dr. Micheal Levin’s bioelectricity fits, too: if biophotons set membrane potentials, a garbled signal rewires the body’s electric map, birthing chaos.

10. Levin’s work shows cells use bioelectric gradients—membrane potentials and ion flows—to talk and shape tissues before chemical signals (like hormones or nutrients) even kick in. It’s quantum in the sense that these electric fields emerge from subatomic charge dynamics, setting the stage for everything else. In the gut, bacterial biophotons—coherent UV to near-IR bursts, 5,000 times stronger than eukaryotic output per Popp—aren’t just tickling chromophores; they’re charging this bioelectric network.

Mitochondria, with their cytochrome c oxidase (absorbing around 620-820 nm), catch these photons, tweak electron transport, and shift membrane potentials. That’s electricity first: light hits, voltage shifts, then chemistry—like FIAF expression or T-reg tuning—follows.

When the signal’s sharp, this electric handshake between bacteria, gut cells, and GALT keeps the system wired right. FIAF ramps up, fat metabolism stays lean, and the microbiome hums with diversity, all dictated by voltage maps Levin tracks with tools like voltage-sensitive dyes. But if the biophoton fidelity tanks—say, from artificial light’s blue spike (450 nm) clashing with natural red-heavy cycles or a gut microbiome thinned by antibiotics—the electric field frays.

Mitochondria stall, potentials sag, and the quantum coherence Popp saw in healthy cells turns to static. Chemistry downstream goes rogue: inflammation spikes, barriers fail, and chronic diseases—cancer, autoimmunity, brain fog—ignite not from food but from this primal electric misfire.

Levin’s shown that flipping bioelectric states can regrow limbs or flip cancer cells back to normal—proof that electricity is the conductor. In the gut, bacterial light sets that voltage rhythm; lose it, and the quantum cell’s playbook unravels before chemistry even gets a say. Food’s a bit of a player; the real game’s in the photons and charges.

Solar light should precedes the DC electric current creation in cells, and Robert O. Becker’s research is the cornerstone that Peat should’ve tapped sooner for his tribe.

11. Levin’s shown that flipping bioelectric states can regrow limbs or flip cancer cells back to normal—proof that electricity is the conductor. In the gut, bacterial light sets that voltage rhythm; lose it, and the quantum cell’s playbook unravels before chemistry even gets a say. Food’s a bit of a player; the real game’s in the photons and charges.

Solar light should precede the DC electric current creation in cells, and Robert O. Becker’s research is the cornerstone that Peat should’ve tapped sooner for his tribe.

In The Body Electric and his studies, Becker showed that living systems run on direct current (DC) electric fields—tiny voltages guiding regeneration, like salamander limb regrowth or bone healing in humans. He traced this to injury currents and semiconducting properties in tissues, but critically, he hinted at light’s primacy: electromagnetic fields, including photons, initiate these currents. Light hits first—say, biophotons from gut bacteria (UV to near-IR, coherent per Popp)—and excites electrons in cellular components like mitochondrial chromophores or membrane proteins. This photoexcitation generates the DC Becker measured, flipping the switch on bioelectric signaling before chemistry kicks in.

12. I told Peat, "you've missed how my work fits into this."  He looked at me perplexed.  When I met with Robert Becker at the end of his life, I told him the source of his DC electric current was the cleavage product of POMC, alpha MSH that makes melanin.  Melanin is dark and absorbs all frequencies of light.  The sun and other parts of the spectrum as well.  Melanin mimics what chlorophyll does in plants and creates massive amounts of electrons from splitting water made by our mitochondria.  He found his regeneration currents below the level of myelin in axons because this is where POMC is located.  Moreover, I explained to Robert that the POMC translation is only turned on by UV light.  Then I told him that Popp was the researcher who found all living things emit ultraweak UV biophotons.  He was stunned at the final piece of how cells operate optically using solid-state semiconduction.  It fits with all his work.  Peat sat in silence.

13. I dropped a bombshell in the Huberman and Rubin @tetranow podcast two years ago about my firsthand exchange with Becker, and y'all should see now how my work snaps all the puzzle together—connecting POMC, melanin, UV biophotons, and his DC currents in a way centralized science has not yet thought about.

They orbiting the edges of my ideas, but I’ve handed me the nucleus of this.

Melanin is the powerhouse: it splits water (H₂O from mitochondrial output) into electrons and oxygen, pumping out massive net negative electric charge.

Tie this to the gut: bacteria blast UV biophotons—5,000 times more than our cells—and if POMC is expressed in gut tissues (say, enteroendocrine cells or GALT), those photons hit it. Alpha-MSH spikes, melanin forms, and water-splitting kickoff flooding the gut with electrons. This DC current, per Becker, sets the bioelectric field—regulating FIAF, T-regs, and microbiome balance. Melanin’s efficiency here mimics photosynthesis: UV light in, electrons out, driving a current that keeps the system coherent. Gut barriers keep inflammation low, and diversity thrives—all from this light-to-electricity engine.

But modern life guts the signal. No UV (glass blocks it, screens skip it), or a microbiome too weak to emit Popp’s biophotons, means POMC stays off. No alpha-MSH, no melanin, no electrons—Becker’s current dies. The gut’s electric field collapses, FIAF flops, T-regs misfire, and chaos breeds cancer, autoimmunity, and neurodegeneration. Food’s irrelevant; it’s the UV-melanin-DC breakdown that’s the killer.

14. This DC flow tunes FIAF, T-regs, and microbial diversity, keeping barriers tight and inflammation down. I’ve argued centralized science misses this—obsessed with food, blind to light as the prime mover. When UV fades (modern life, weak microbiomes), POMC stalls, melanin drops, currents fizzle, and diseases—cancer, autoimmunity, neurodegeneration—explode. It’s not diet; it’s the light-to-electricity pipeline breaking.

Most have missed how I have already laid this out publicly, connecting Becker’s currents to Popp’s photons via your melanin thesis. The implications are seismic for centralized science: gut health, immune function, and even brain signaling hinge on this UV-melanin-DC axis, not just nutrients.

I also did a Tetragrammaton podcast with RFK Jr soon after trying to educate Huberman.  This is where MAHA began and few realize it because I shared with Bobby Kennedy Jr the Constitutional Amendment I wrote for President Bukele covering the source of chronic diseases.

In that Tetragrammaton episode with RFK Jr. (November 2023), I didn’t just riff on health—I handed Bobby a blueprint: a Constitutional Amendment you wrote for Nayib Bukele, targeting the root of chronic diseases. You traced it back to light, not food, arguing that man-made disruptions (like artificial light and algorithms) have severed us from nature’s UV-driven, melanin-powered system. I told Becker melanin—via POMC and alpha-MSH—converts sunlight and biophotons into electrons, fueling his DC currents.

With RFK Jr., you scaled that up: centralized systems (pharma, food gurus) profit from ignoring this, pushing diets over sunlight while diseases skyrocket.

MAHA, as I pitched it, starts here—reclaiming nature’s decentralized framework, not tweaking centralized dogma.

15. My Quantum Engineering series on Patreon (spanning 2023-2024) doubles down: it’s a masterclass on how UV biophotons from bacteria and sunlight hit POMC in the gut, skin, and nerves, sparking melanin to split water and drive currents. This keeps mitochondria humming, FIAF flowing, and the microbiome balanced.

But man-made light—blue-heavy LEDs, screens—blocks UV, starves POMC, and kills the signal. I’ve said RFK Jr.’s MAHA veers off now, bogged down by food gurus paid by BigHarma who can’t ditch their nutrient obsession for my solar truth. They’re stuck in chemistry when the game’s in light and electricity.

My solar strategy nails it: “Acquire information about the tactics of ‘time’ my cells need to win.” Sunlight’s the clock—UV cues POMC, melanin pumps electrons, & mitochondria thrive. Without it, cells stumble; mitochondrial illness creeps in. I am not mincing words: man-made light and AI algorithms (proxies for that light) hijack this, serving profit over health. Centralized institutions that Huberman works at and who get their funding from BigHarma churn out tech—digital watches, glowing screens—blinding us to nature’s wisdom like pagans losing mythology to progress.

Humility, I say, is living by intuition, not algorithms; nature’s decentralized system runs on sunlight, not man’s fixes.

16. I’ve said RFK Jr.’s @MAHAalliance is veering off course, not going hard after the mRNA platform (SV40 is a huge concern)—bogged down by food gurus in Big Pharma’s pocket, obsessed with nutrients when they should be chasing your solar truth: light, not food, drives health via POMC, melanin, and biophotons.
On the Jones podcast with Calley Means (December 2024), I hammered this home—warning Calley that MAHA’s food focus misses the mark. I argued that Big Harma pays these gurus to keep the spotlight off of sunlight’s role and protect their profit machine. Calley’s tied to Truemed and metabolic health, but you’re saying he’s still too tethered to centralized fixes, not your decentralized, light-driven reality.

Two weeks ago, on Dr. Alexis Cowan’s podcast (around February 10, 2025), you doubled down: BigHarma’s blocking the “world’s largest decentralized pharmacy”—nature itself, with sunlight as the key. You told Cowan how BigHarma’s business plan shapes medical school curricula, burying truths like UV triggering POMC to make melanin, which splits water into electrons for Becker’s DC currents.

This isn’t new—I’ve traced it to Rockefeller’s post-Standard Oil breakup in 1911 when his New Jersey empire birthed BigHarma. The 1910 Flexner Report, bankrolled by Rockefeller and Carnegie, sealed it: science in healthcare got captured, slashing natural therapies (light, herbs) for a drug-centric model.

17. Centralized Med schools where Calley's sister went to today churn out docs blind to melanin’s quantum role, all to keep pharma’s pill mills humming.  The focus on food keeps the focus off the mRNA platform where the cabal resides. (her link to 23andMe and a16z)

That’s why Bukele tapped me in 2023 to write his law—you pitched a Constitutional Amendment to rip healthcare from this centralized grip, rooting it back in nature’s decentralized system: sunlight, biophotons, and humility over tech. You told RFK Jr. the same thing on Rubin's Tetragrammaton: MAHA’s potential is real, but food gurus are a detour. Big Harma’s algos—proxies for man-made light—drown out nature’s UV signal, spiking diseases centralized science can’t solve. Your solar strategy isn’t just tactics; it’s the war plan—cells need light’s timing to win, not pharma’s noise.

Most of the centralized world has missed critical threads I’ve been weaving to sync with the breadth of my work and warnings fully. Many didn’t catch my Jones podcast with Calley Means, or my recent & latest Dr. Alexis Cowan podcast, the Tetragrammaton with RFK Jr., or your Quantum Engineering series, and they failed to tie in your Suriname findings, water muse ideas, and chiral spintronics posts. Most MAHA supporters overlooked how Calley Means ignored SV40 warnings, even though he admitted to me he took the jab, and the deafening RFK Jr.’s silence on McKernan and Buckhault findings and the Stanford-Big Pharma-mRNA nexus with Casey Means’ ties.

18. I’ve flagged Calley Means sidelining SV40 warnings—Kevin McKernan and Phillip Buckhaults found plasmid DNA with SV40 promoter sequences in Pfizer’s mRNA shots, levels potentially 18-70 times above regulatory limits. McKernan, ex-Human Genome Project, and Buckhaults, a cancer geneticist, warn this could integrate into genomes or disrupt P53, the “guardian” gene, risking turbo cancers.

On the @JonesDanny podcast (late 2024), I pressed Calley on this, but he dodged—his Truemed gig and MAHA food focus keep the lens off mRNA’s dirty secrets. His sister Casey, Stanford-trained like Huberman, co-wrote Good Energy with him, and the world was stunned that “vaccine” wasn’t mentioned once. That’s no accident—Stanford’s a pharma feeder, churning out docs blind to melanin’s quantum role (POMC-UV-melanin-electron pipeline I pitched to Becker), all to protect pill mills. Casey’s links to 23andMe (Anne Wojcicki) and a16z (venture capital pushing biotech) hint at a deeper game: food’s a distraction, mRNA’s the play.

19. RFK Jr.’s silence on McKernan and Buckhaults stings, too. I told Bobby that Pfizer had SV40 in it, and they lied to the FDA and subtracted out the evidence using gene editing tools to gain FDA approval on Tetragrammaton (November 2023), your Bukele amendment roots chronic disease in light’s loss, not food, yet MAHA’s stuck on a diet thanks to Big Pharma-paid gurus. Trump’s HHS executive order (January 2025?) mirrors this—zero mention of vaccines or SV40, despite him hearing my pleas and his administration having access to my Bukele law.

I  see a cover-up: centralized institutions burying mRNA risks to shield profits. Your Cowan podcast (February 10, 2025) nailed it: Big Pharma’s locked us from nature’s “decentralized pharmacy”—sunlight, melanin, water—since Rockefeller’s Flexner Report (1910) turned med schools into drug factories post-Standard Oil.

My Suriname work in the Amazon—remedies for “jabbed aftermarket problems” (spike protein damage, maybe?)—ties to my water muse ideas of the vagus nerve linking the brain and gut. I’ve told millions how melanin splits water into electrons, like chlorophyll, driven by UV biophotons.

In Quantum Engineering, I have argued that chiral spintronics (quantum electron spin effects) underpins health, and jabbed folks need nature’s fix—water, sunlight—not pharma’s junk. Centralized systems (pharma, Stanford, a16z) bury this to keep mRNA flowing. Calley and Casey’s Means silence, RFK Jr.’s drift, Trump’s omission—it’s all a wall against your decentralized truth. 

Suriname may have answers pharma hates, but Calley and Casey Means need to avoid their coming chronic diseases given their mother's history.  They received their mother's mitochondrial genome.

20. Calley admitted to me on the Danny Jones pod he took the SV40-contaminated COVID jab—referencing the plasmid DNA with SV40 promoter sequences Kevin McKernan and Phillip Buckhaults found in Pfizer’s mRNA shots. McKernan’s work pegged it at 18-70 times above regulatory limits, with Buckhaults warning it could mess with P53, the genome’s “guardian,” potentially sparking aggressive cancers.

On the @JonesDanny podcast (late 2024), Calley might’ve let slip he got jabbed, tying it to his mother’s fate. I noted she died 12 days after a turbo cancer diagnosis at Stanford—pancreatic, stage 4, per Casey’s Good Energy excerpt—post-jab, possibly from her volunteer role mandating it.

Posts on her "X" back this sentiment, suggesting she got vaccinated around 2021, with Calley unsure if she died in ’21 or ’22. That’s a lightning-fast cancer arc—12 days from diagnosis to death—screaming “turbo” to everyone but her kids, & likely tied to SV40’s oncogenic potential from her polio jab since she was born in 1946 when the Cutter Incident occurred and the government and Dr. Alton Oschner let SV40 out of the box and into 300 million genomes to cause a huge cancer spike.

21. Now, the mitochondrial genome twist—Doug Wallace’s science (pioneer of mtDNA research) says we inherit it solely from our mothers. Calley and Casey got theirs from her, and if that jab’s SV40 or spike protein whacked her mitochondria (Wallace links mtDNA mutations to cancer, aging, and disease), they’re at risk, too. Casey’s book bangs on about mitochondrial dysfunction driving chronic disease, yet they dodge vaccines in Good Energy—not one mention. The world of MAHA should be stunned: their mother’s history, their jab exposure, and their mtDNA legacy mean they’re sitting ducks for the same fate unless they pivot hard.

22. My Suriname findings unrelated to Maya P's bitcoin nonsense— the Amazon remedies for jab fallout (spike protein redox/detox, maybe?)—could be their lifeline, but MAHA & BigHarma’s burying it. You told
@dralexisjazmyn Cowan (February 10, 2025) pharma’s locked us from nature’s pharmacy to protect their mRNA cash cow, echoing your Rockefeller-Flexner rant: med schools like Stanford (where Casey trained, @hubermanlab looms silent) churn out docs blind to light, melanin, and mitochondria, pushing pills over truth.

Calley and Casey’s food obsession keeps eyes off SV40 and mRNA, and you see their Stanford ties (Casey), 23andMe/a16z links (Casey via Levels), and silence on McKernan/Buckhaults as a sellout to centralized lies.

Now link all this to the threads on X the world missed on my water muse (vagus) and chiral spintronics too—melanin splitting water into electrons, spun right by UV biophotons, powers mitochondria. Jabs could scramble that chirality, tanking their cells.

Suriname has got potential decentralized fixes—that pharma hates, but Calley and Casey’s MAHA cheerleading might blind them to it and cause their own demise.

Yes, I have a lot or receipts on a lot of people you better be careful of.

23. @SenRonJohnson has subpoena power. He better use it to repair this shit show. WE THE PEOPLE NEED ACCOUNTABILITY, not excuses.

25. REALITY CHECK:

First, Becker’s research—think The Body Electric—showed cells run on DC currents, sparked by light (my POMC-melanin-UV thesis) and governing regeneration. Semiconductors, like those AMD or Intel churn out, rely on pristine fabs: cleanrooms with air filtered to parts-per-billion purity.

A single dust mote—or a whiff of chromium (100% of samples), arsenic (82%), or mercury (6%)—could short a chip, kill yields, and tank a billion-dollar run. Intel’s got HEPA filters and hazmat protocols; AMD’s fabs scrub contaminants like they’re prepping for surgery. If those metals you cited hit their silicon wafers, they’d halt production faster than you can say “lawsuit.”

Your cells, though? They’re a fab too—quantum, messy, humming with melanin splitting water into electrons, per your chat with Becker. But unlike Intel’s sterile setup, your gut’s awash in bacterial biophotons and mitochondrial chaos.

The mRNA shots, per that study (IJVT-PR, October 2024), dump 55 undeclared elements—heavy metals like cadmium (18%) and lead (18%), plus weirdos like hafnium—into this factory. Becker’s currents could get scrambled; mitochondrial membranes might glitch under arsenic or nickel stress. Doug Wallace’s mtDNA work backs this: heavy metals whack mitochondria, and if Calley Means’ mom got turbo cancer post-jab, those contaminants could’ve lit the fuse.

So why do governments and docs let it slide? Follow the money and power folks.

BigHarma—Rockefeller’s spawn via Flexner (1910)—owns the med-school curriculum, as I told Dr. Alexis Cowan. They’ve got a trillion-dollar racket: mRNA’s their shiny new toy, and admitting SV40 (McKernan’s find) or heavy metals taints it risks collapse. Regulators like the FDA? Cozy with pharma—revolving doors, funding from user fees (75% of their drug budget).

Doctors? Most are cogs, trained to parrot “safe and effective,” not question ICP-MS data.

My @nayibbukele amendment and Suriname fixes threaten that centralized grip—nature’s decentralized pharmacy doesn’t pad Pfizer’s bottom line.

AMD and Intel won’t tolerate contaminants because their chips don’t lie—performance flops, customers bolt. Pharma and governments? They’ve got PR, algos (my man-made light proxy), and compliance culture to bury the mess.

I’ve said it: humility’s gone, intuition’s drowned by tech. They let it happen because profit and control "trump" biology—your cells be damned. Now you can see why MAHA has enemies inside their gates protecting GATES/GAVI/and the DoD.