Yes, the chronic accumulation of deuterium from a high-sugar diet under isolated artificial blue light acts as a direct, physical cause for the eventual burnout and death of pancreatic beta cells in long-term Type II diabetes.
Through my four-pillar framework, this process is not an abstract biochemical pathway. It is a predictable thermodynamic breakdown of the beta cell's internal LC oscillator, culminating in an irreversible Landauer liquidation where insulin production drops to zero.
Pancreatic beta cells function as the ultimate glucose sensors of the human body. They regulate insulin secretion not by counting molecules, but by tracking the exact rate of mitochondrial ATP production. When a patient consumes high-sugar carbohydrates (specifically sucrose and high-fructose corn syrup) under artificial blue light, they create a destructive physical feedback loop:
The High-Sugar Isotope Load: Processed sugars are highly deuterated. Plants pack deuterium into their storage carbohydrates. When consumed, these sugars flood the cytoplasm of the beta cell with an immense concentration of heavy mass D+.
The Blue Light Dielectric Crash: Exposure to isolated, non-native blue light (from screens and LED bulbs) lacks the balancing infrared red photons needed to build structured water. As blue light excites the local tissues, it shatters the hydrogen-bond matrix of cellular water.
The beta cell's internal water table drops from its polarized ferroelectric state (K= 160 straight down to chaotic bulk water ----> 78). With the dielectric constant cut in half, the cell's ability to exclude heavy isotopes disappears because NADD+ and singlet oxygen drop the IMM charge from 30 million volts. The un-pruned deuterium is drawn directly into the cytosol and into the matrix of the mitochondria to deuterate NAD+, destroying redox power.
Inside the beta cell, glucose undergoes glycolysis and oxidative phosphorylation to produce ATP. The rising ratio of ATP to ADP is what forces the cell's ATP-sensitive K+ channels to close, depolarizing the cell membrane, opening voltage-gated Ca2+ channels, and triggering the rapid exocytosis of insulin granules. K+ is what creates the 160 dielectric with melanin's help.
The ATP synthase nanomotor is a spinning quantum rotor engineered to run exclusively on light, single-proton hydrogen (H+). When a heavy deuterium ion (D+) enters the channel, its double inertial mass shatters the frictionless Brachistochrone cycloid track of the IMJ. The rotor experiences immediate physical and quantum friction, causing the nanomotor to lag, stall, or mechanically break.
Because the nanomotors are broken by the heavy-mass "grease," the beta cell’s capacity to generate ATP collapses. The ATP/ADP ratio fails to spike, the membrane cannot depolarize, and the cell can no longer push insulin out into the bloodstream. Centralized medicine calls this "beta-cell fatigue" from over-secretion. In reality, the beta cell is full of manufactured insulin, but the quantum mechanical trigger, the ATP stroke, is jammed by isotopic mass.
Because the stalled electron transport chain can no longer route energy cleanly into metabolic work, the electromagnetic grip of the fine-structure constant (alpha{bio}) slips from its ideal (1/137) threshold. The uncoupled energy leaks into the intracellular matrix as chaotic, high-entropy thermal friction.
This triggers The Singlet Trap: oxygen atoms within the cell are continuously kicked into a highly volatile singlet state. This localized oxidative fire cooks the beta cell from the inside out, damaging its transcriptome and forcing it to undergo dedifferentiation (losing its functional identity). To protect the surrounding pancreatic architecture from this runaway thermodynamic fire, the body executes a localized Landauer liquidation. The chronically deuterated, non-functional beta cells are systematically purged via apoptosis. Centralized medicine teaches that once these physical oscillators are erased, the long-term Type II diabetic permanently loses the capacity to produce endogenous insulin. I do not. I understand that the beta cell stem cells can regenerate the function via photorepair mechanisms built by Robert O. Becker's work.
The sun reduces BG by 29% and deuterium depletes the beta cells. The ultimate clinical proof of this causal relationship is observed when this exact thermodynamic loop is reversed. Peer-reviewed metabolic research has documented long-term, advanced Type II diabetic patients achieving rapid improvements in glucose tolerance, reduced HbA1c, and a spontaneous restoration of pancreatic insulin secretion through the implementation of systemic deuterium depletion.
The pancreatic beta cell is not a victim of a genetic programming error. It is a decentralized electrical circuit operating on a physical stage. When you load it with the high mass of sugar (D+) and expose it to the dielectric-shattering frequency of artificial blue light, it experiences the exact same Lattice Lock failure that collapsed the vineyards of Europe after the Carrington Event. The symphony is identical: to save the base oscillator, you must prune the superfluous mass and restore the ordered dielectric stage.
The Rockerfeller dynasty has taught MDs that diabetes is not reversible. Guess why? they knew they were making GLP1a's in the 1980s. An MD nmae Dr. Alo is a perfect analolgy of Rockefeller medicine. He spews this nonsense all the time. He is a retard.
In a decentralized system, you cannot analyze a jammed motor without looking at its tailpipe. The pancreatic beta cell is not just an ATP sensor; it is a primary anatomical terminal for the vagal exhaust system, where carbon dioxide and water are converted into bicarbonate to flush out the heavy, high-entropy atomic mass (D+) before it induces a systemic Lattice Lock in the cell's water table.
The pancreas is heavily innervated by the vagus nerve, which directly controls the secretion of both insulin and bicarbonate. Bicarbonate is the body's ultimate physical transformer, it is a carbon-based negative charge carrier designed to buffer protons and maintain the local fluidic dielectric constant. In a healthy state with a strong planetary Magnetic-field, the vagus nerve drives the enzyme carbonic anhydrase. This enzyme takes metabolic waste CO2 and combines it with light cellular water (H2O) to synthesize HCO3-. Because bicarbonate carries a heavy negative charge, it acts as a magnet for positive ions. It binds the heavy, high-entropy deuterium (D+) "grease" and sweeps it out of the cellular matrix into the pancreatic ducts. This keeps the mitochondrial water table at a pristine (k = 160) baseline.
When you introduce a high-sugar diet under isolated blue light, or a magnetic excursion, the dielectric constant collapses to (k= 78). The water thickens, viscosity spikes, and the carbonic anhydrase enzyme loses its quantum spin-alignment. The cell can no longer form or export bicarbonate efficiently. The tailpipe is effectively welded shut. This are the boundary conditions created by Rockefeller biotech since the 1940s.
The Backup: Because the (HCO3-) exhaust cannot clear, the heavy D+ mass backs up directly into the beta cell's mitochondrial matrix, stalling the ATP synthase rotors, causing the uncoupled energy to leak as singlet oxygen fire, and terminating insulin production.
Centralized medicine tells diabetics they must manage their disease by micromanaging their carbohydrate infusions, cutting out sugars or calculating insulin units. My thesis shows that this is an ungrounded, material-only band-aid. If you understand that the root cause is a blocked exhaust pipe driving an artificial mass overload, you realize that if you can mechanically clear the vagal HCO3- exhaust, the cell will naturally clear its own diabetes, regardless of carbohydrate intake. There are two macro-scale forces capable of clearing this pipe without diet restrictions:
1. Way one: By utilizing active phase-conjugate systems—like My Leptin Rx or the Melanin Renovation Rx or understanding how to build custom Spurling/Lakhovsky electromagnetic resonance fields positioned precisely over the vagal choke point at the neck and the solar plexus, you introduce a highly ordered longitudinal wave column.
2. Introduction of DDW, 3%NaCl and use of triplet state oxygen to cause an instant drop in viscosity clears the friction in the carbonic anhydrase pathway. Bicarbonate production skyrockets, immediately binding the trapped deuterium mass and dragging it out through the pancreatic exhaust. The ATP synthase motors are cleared of grease, resume spinning at near-superfluid speeds, and insulin sensitivity restores itself spontaneously.
Through my four-pillar framework, this process is not an abstract biochemical pathway. It is a predictable thermodynamic breakdown of the beta cell's internal LC oscillator, culminating in an irreversible Landauer liquidation where insulin production drops to zero.
Pancreatic beta cells function as the ultimate glucose sensors of the human body. They regulate insulin secretion not by counting molecules, but by tracking the exact rate of mitochondrial ATP production. When a patient consumes high-sugar carbohydrates (specifically sucrose and high-fructose corn syrup) under artificial blue light, they create a destructive physical feedback loop:
The High-Sugar Isotope Load: Processed sugars are highly deuterated. Plants pack deuterium into their storage carbohydrates. When consumed, these sugars flood the cytoplasm of the beta cell with an immense concentration of heavy mass D+.
The Blue Light Dielectric Crash: Exposure to isolated, non-native blue light (from screens and LED bulbs) lacks the balancing infrared red photons needed to build structured water. As blue light excites the local tissues, it shatters the hydrogen-bond matrix of cellular water.
The beta cell's internal water table drops from its polarized ferroelectric state (K= 160 straight down to chaotic bulk water ----> 78). With the dielectric constant cut in half, the cell's ability to exclude heavy isotopes disappears because NADD+ and singlet oxygen drop the IMM charge from 30 million volts. The un-pruned deuterium is drawn directly into the cytosol and into the matrix of the mitochondria to deuterate NAD+, destroying redox power.
Inside the beta cell, glucose undergoes glycolysis and oxidative phosphorylation to produce ATP. The rising ratio of ATP to ADP is what forces the cell's ATP-sensitive K+ channels to close, depolarizing the cell membrane, opening voltage-gated Ca2+ channels, and triggering the rapid exocytosis of insulin granules. K+ is what creates the 160 dielectric with melanin's help.
The ATP synthase nanomotor is a spinning quantum rotor engineered to run exclusively on light, single-proton hydrogen (H+). When a heavy deuterium ion (D+) enters the channel, its double inertial mass shatters the frictionless Brachistochrone cycloid track of the IMJ. The rotor experiences immediate physical and quantum friction, causing the nanomotor to lag, stall, or mechanically break.
Because the nanomotors are broken by the heavy-mass "grease," the beta cell’s capacity to generate ATP collapses. The ATP/ADP ratio fails to spike, the membrane cannot depolarize, and the cell can no longer push insulin out into the bloodstream. Centralized medicine calls this "beta-cell fatigue" from over-secretion. In reality, the beta cell is full of manufactured insulin, but the quantum mechanical trigger, the ATP stroke, is jammed by isotopic mass.
Because the stalled electron transport chain can no longer route energy cleanly into metabolic work, the electromagnetic grip of the fine-structure constant (alpha{bio}) slips from its ideal (1/137) threshold. The uncoupled energy leaks into the intracellular matrix as chaotic, high-entropy thermal friction.
This triggers The Singlet Trap: oxygen atoms within the cell are continuously kicked into a highly volatile singlet state. This localized oxidative fire cooks the beta cell from the inside out, damaging its transcriptome and forcing it to undergo dedifferentiation (losing its functional identity). To protect the surrounding pancreatic architecture from this runaway thermodynamic fire, the body executes a localized Landauer liquidation. The chronically deuterated, non-functional beta cells are systematically purged via apoptosis. Centralized medicine teaches that once these physical oscillators are erased, the long-term Type II diabetic permanently loses the capacity to produce endogenous insulin. I do not. I understand that the beta cell stem cells can regenerate the function via photorepair mechanisms built by Robert O. Becker's work.
The sun reduces BG by 29% and deuterium depletes the beta cells. The ultimate clinical proof of this causal relationship is observed when this exact thermodynamic loop is reversed. Peer-reviewed metabolic research has documented long-term, advanced Type II diabetic patients achieving rapid improvements in glucose tolerance, reduced HbA1c, and a spontaneous restoration of pancreatic insulin secretion through the implementation of systemic deuterium depletion.
The pancreatic beta cell is not a victim of a genetic programming error. It is a decentralized electrical circuit operating on a physical stage. When you load it with the high mass of sugar (D+) and expose it to the dielectric-shattering frequency of artificial blue light, it experiences the exact same Lattice Lock failure that collapsed the vineyards of Europe after the Carrington Event. The symphony is identical: to save the base oscillator, you must prune the superfluous mass and restore the ordered dielectric stage.
The Rockerfeller dynasty has taught MDs that diabetes is not reversible. Guess why? they knew they were making GLP1a's in the 1980s. An MD nmae Dr. Alo is a perfect analolgy of Rockefeller medicine. He spews this nonsense all the time. He is a retard.
In a decentralized system, you cannot analyze a jammed motor without looking at its tailpipe. The pancreatic beta cell is not just an ATP sensor; it is a primary anatomical terminal for the vagal exhaust system, where carbon dioxide and water are converted into bicarbonate to flush out the heavy, high-entropy atomic mass (D+) before it induces a systemic Lattice Lock in the cell's water table.
The pancreas is heavily innervated by the vagus nerve, which directly controls the secretion of both insulin and bicarbonate. Bicarbonate is the body's ultimate physical transformer, it is a carbon-based negative charge carrier designed to buffer protons and maintain the local fluidic dielectric constant. In a healthy state with a strong planetary Magnetic-field, the vagus nerve drives the enzyme carbonic anhydrase. This enzyme takes metabolic waste CO2 and combines it with light cellular water (H2O) to synthesize HCO3-. Because bicarbonate carries a heavy negative charge, it acts as a magnet for positive ions. It binds the heavy, high-entropy deuterium (D+) "grease" and sweeps it out of the cellular matrix into the pancreatic ducts. This keeps the mitochondrial water table at a pristine (k = 160) baseline.
When you introduce a high-sugar diet under isolated blue light, or a magnetic excursion, the dielectric constant collapses to (k= 78). The water thickens, viscosity spikes, and the carbonic anhydrase enzyme loses its quantum spin-alignment. The cell can no longer form or export bicarbonate efficiently. The tailpipe is effectively welded shut. This are the boundary conditions created by Rockefeller biotech since the 1940s.
The Backup: Because the (HCO3-) exhaust cannot clear, the heavy D+ mass backs up directly into the beta cell's mitochondrial matrix, stalling the ATP synthase rotors, causing the uncoupled energy to leak as singlet oxygen fire, and terminating insulin production.
Centralized medicine tells diabetics they must manage their disease by micromanaging their carbohydrate infusions, cutting out sugars or calculating insulin units. My thesis shows that this is an ungrounded, material-only band-aid. If you understand that the root cause is a blocked exhaust pipe driving an artificial mass overload, you realize that if you can mechanically clear the vagal HCO3- exhaust, the cell will naturally clear its own diabetes, regardless of carbohydrate intake. There are two macro-scale forces capable of clearing this pipe without diet restrictions:
1. Way one: By utilizing active phase-conjugate systems—like My Leptin Rx or the Melanin Renovation Rx or understanding how to build custom Spurling/Lakhovsky electromagnetic resonance fields positioned precisely over the vagal choke point at the neck and the solar plexus, you introduce a highly ordered longitudinal wave column.
2. Introduction of DDW, 3%NaCl and use of triplet state oxygen to cause an instant drop in viscosity clears the friction in the carbonic anhydrase pathway. Bicarbonate production skyrockets, immediately binding the trapped deuterium mass and dragging it out through the pancreatic exhaust. The ATP synthase motors are cleared of grease, resume spinning at near-superfluid speeds, and insulin sensitivity restores itself spontaneously.
https://x.com/DrJackKruse/status/2062678091143557438
2. To understand insulinoma one must reject billard ball biochemistry for biophysics. Why?
Applying a biophysical layer directly to the pancreatic beta-cell reveals why the tumor displays its unique autonomous signature:
Fat is The Deuterium-Depleted "High-Dielectric" Magnetic Fuel
As the slide below states, 100g of fat yields 110g of metabolic water. The Isotopic Advantage: Fat (Beta-oxidation) produces significantly more DDW per gram than any other substrate. It is the "Coolant" of the human semiconductor when it is creating heat when the IMM is making singlet free radicals.
When NAD+ becomes NADD+ the buffer is gone and triplet oxygen becomes singlet oxygen and billard ball biochemistry misses how that changes the 30 million volt charge (Nick Lane) on the IMM that begins to allow D+ into the cell's water table lattice first in the cytosol and as the charge drops as the electromagnetic pull from NADD+ to singlet oxygen degrades leads to an effective shortening of the IMM and loss of voltage. D+ surges into the cytosol and matric leading to heteroplasmy = Warburg shift that leads to atavism and cell growth because the UPE signal is altered altering cell cycle kinetics.
This is all biophysical and missed by centralized biochemistry because of the Flexner curricula change as a boundary condition for centralized medicine. This consensus change supported a huge shift support Pharma over physics for profiteering of drug sales. Understanding water table dielectric changes on physiciology requires a Physics over pharma consensus mechanism.
From this biophysical perspective, an insulinoma is not just a collection of random mutations; it is a macroscopic adaptation to a localized collapse of the cellular semiconductor lattice and its dielectric "water table."
When the 30 million volt capacitor drops its charge, the biophysical barrier preventing heavier isotopes from entering the mitochondrial matrix is lost.
Heteroplasmy and the Kinetic Jam: Heavy hydrogen (D+) floods the cytosol and matrix, mechanically jamming the rotating nanomotors of ATP synthase (which are physically calibrated for the kinetic mass of (H+). This kinetic breakdown forces a permanent transition to cytoplasmic glycolysis, the classic Warburg Shift.
Atavism and Ultra-Weak Photon Emission (UPE): In biophysics, when a cell cannot maintain its mitochondrial dielectric potential, it loses its coherent quantum signaling. The altered coherent light or Ultra-Weak Photon Emission (UPE) changes cell cycle kinetics. The cell reverts to an ancient, atavistic survival program: rapid, autonomous proliferation (tumor growth) designed to escape a locally toxic, heavy-hydrogen environment.
The Bicarbonate/Proton Uncoupling: The beta-cell relies on tight electro-chemical gradients to store insulin inside secretory granules. When the localized water table is contaminated by D+ and the IMM voltage drops, the bicarbonate clearance loop degrades.
Unregulated Quantum Leak: The beta-cell can no longer read the localized electronic signature of blood glucose. The machinery that should destroy unneeded insulin fails because the structural pH balance is lost. Instead of maintaining control, the damaged semiconductor grid continuously discharges its cargo, resulting in the clinical reality of chronic hypoglycemia and Whipple's Triad.
I've correctly identify that this biophysical perspective was largely minimized following the standardization of medical education via the Flexner Report framework. By prioritizing a biochemical "lock-and-key" model, centralized medicine focused on isolating individual proteins, receptors, and downstream drug targets. This is why we are being sold the deadly GLP1A now. More on that in other threads (magnetic pinning thread in Factor X part of the forum)
This biochemical lens overlooks the thermodynamic boundary conditions, such as the submolecular D+/H+ ratio, mitochondrial field strength, and the dielectric properties of water, that dictate whether a cell maintains its differentiated state or drops into an atavistic growth phase. More deuterium = insulinoma is likely once insulin secretion is show down due to deuteration of the beta cell. Insulinoma will explode with RETA use. Mark my words.
SUMMARY
An insulinoma is the macroscopic manifestation of a localized dielectric breakdown. When the cell loses its ability to generate deuterium-depleted metabolic water from fat, singlet oxygen destroys the IMM charge, allowing a D+ surge to shift the beta-cell into a permanent Warburg state of autonomous proliferation.
Applying a biophysical layer directly to the pancreatic beta-cell reveals why the tumor displays its unique autonomous signature:
Fat is The Deuterium-Depleted "High-Dielectric" Magnetic Fuel
As the slide below states, 100g of fat yields 110g of metabolic water. The Isotopic Advantage: Fat (Beta-oxidation) produces significantly more DDW per gram than any other substrate. It is the "Coolant" of the human semiconductor when it is creating heat when the IMM is making singlet free radicals.
When NAD+ becomes NADD+ the buffer is gone and triplet oxygen becomes singlet oxygen and billard ball biochemistry misses how that changes the 30 million volt charge (Nick Lane) on the IMM that begins to allow D+ into the cell's water table lattice first in the cytosol and as the charge drops as the electromagnetic pull from NADD+ to singlet oxygen degrades leads to an effective shortening of the IMM and loss of voltage. D+ surges into the cytosol and matric leading to heteroplasmy = Warburg shift that leads to atavism and cell growth because the UPE signal is altered altering cell cycle kinetics.
This is all biophysical and missed by centralized biochemistry because of the Flexner curricula change as a boundary condition for centralized medicine. This consensus change supported a huge shift support Pharma over physics for profiteering of drug sales. Understanding water table dielectric changes on physiciology requires a Physics over pharma consensus mechanism.
From this biophysical perspective, an insulinoma is not just a collection of random mutations; it is a macroscopic adaptation to a localized collapse of the cellular semiconductor lattice and its dielectric "water table."
When the 30 million volt capacitor drops its charge, the biophysical barrier preventing heavier isotopes from entering the mitochondrial matrix is lost.
Heteroplasmy and the Kinetic Jam: Heavy hydrogen (D+) floods the cytosol and matrix, mechanically jamming the rotating nanomotors of ATP synthase (which are physically calibrated for the kinetic mass of (H+). This kinetic breakdown forces a permanent transition to cytoplasmic glycolysis, the classic Warburg Shift.
Atavism and Ultra-Weak Photon Emission (UPE): In biophysics, when a cell cannot maintain its mitochondrial dielectric potential, it loses its coherent quantum signaling. The altered coherent light or Ultra-Weak Photon Emission (UPE) changes cell cycle kinetics. The cell reverts to an ancient, atavistic survival program: rapid, autonomous proliferation (tumor growth) designed to escape a locally toxic, heavy-hydrogen environment.
The Bicarbonate/Proton Uncoupling: The beta-cell relies on tight electro-chemical gradients to store insulin inside secretory granules. When the localized water table is contaminated by D+ and the IMM voltage drops, the bicarbonate clearance loop degrades.
Unregulated Quantum Leak: The beta-cell can no longer read the localized electronic signature of blood glucose. The machinery that should destroy unneeded insulin fails because the structural pH balance is lost. Instead of maintaining control, the damaged semiconductor grid continuously discharges its cargo, resulting in the clinical reality of chronic hypoglycemia and Whipple's Triad.
I've correctly identify that this biophysical perspective was largely minimized following the standardization of medical education via the Flexner Report framework. By prioritizing a biochemical "lock-and-key" model, centralized medicine focused on isolating individual proteins, receptors, and downstream drug targets. This is why we are being sold the deadly GLP1A now. More on that in other threads (magnetic pinning thread in Factor X part of the forum)
This biochemical lens overlooks the thermodynamic boundary conditions, such as the submolecular D+/H+ ratio, mitochondrial field strength, and the dielectric properties of water, that dictate whether a cell maintains its differentiated state or drops into an atavistic growth phase. More deuterium = insulinoma is likely once insulin secretion is show down due to deuteration of the beta cell. Insulinoma will explode with RETA use. Mark my words.
SUMMARY
An insulinoma is the macroscopic manifestation of a localized dielectric breakdown. When the cell loses its ability to generate deuterium-depleted metabolic water from fat, singlet oxygen destroys the IMM charge, allowing a D+ surge to shift the beta-cell into a permanent Warburg state of autonomous proliferation.
3. Precursor to the monster tweet.
4. This response is taken right from my work on Patreon.
The Nazis weren't inventing a new physics; they were attempting to mechanize and compress the passive macroscopic space-time regulation methods of the ancients into a mobile, high-voltage active antigravity device. A lot of this data made it through Operation Paperclip, NASA, DARPA, and into the space program.
The Ancient Method (Teotihuacan & China): They used vast, static quantities of liquid mercury laid out in subterranean river paths under heavy geometric capacitors. They relied on mercury's natural relativistic electronic density and raw volume mass (13.53g/cm^3) to passively pin magnetic flux and hold local space-time order.
The SS realized they could bypass the need to build a literal pyramid or dig a massive lake by introducing macroscopic rotational spin-quanta. By taking a mercury-based liquid (Xerum 525) and forcing it through two counter-rotating cylinders at hyper-high RPMs under extreme high-voltage electrical excitation, they artificially multiplied the local energy density vector by orders of magnitude.
By spinning the mercury in opposing directions, they achieved Common Mode Rejection. The transverse components of the massive electromagnetic currents crashed directly into one another and nullified. This forced a massive centripetal wave implosion, compressing the local magnetic-field into an intensely focused, longitudinal column.
The strategic goal of Die Glocke under Hans Kammler was not simply to make a weapon, but to construct a Timeline Disruptor and Reality Anchor. By driving the ordered component of local energy density to structural extremes inside the Bell, they aimed to completely decouple the interior chamber from the background planetary time-flow. They knew about the ancient megalith sites use of physics to do the same during excursions. I found evidence of this in the MKULTRA boxes in Charity Hospital.
Why was the link made?
Plotner told Groves about the use of amphetamines in the SS to Groves. He relayed it was done to mind control soldiers to better performance and the process began and was field tested in the 1939 Olympics. Big Harma complany Temmler patented and launched Pervitin in 1938 after studying Mexican peyote, and through an alliance with the Wehrmacht and the SS high command, they supplied tens of millions of tablets to fuel atheletes and soldiers in WW2 to power the mind to perform under sleepless, to facilitate the high-velocity campaigns of the Blitzkrieg.
What did the Nazi Plotner relay to Groves via Lansky? Through the lens of my decentralized thesis, the pharmacology of Pervitin reveals a profound, synthetic hijacking of the body's peripheral POMC clipping architecture and energy-density regulators. This was how the SCN melanin RPE became a target of the Nazi's. They realized melanin was paramagnetic and it was chiral and it was dram to magnetic fields. These Hg experiments and the link to melanin was made by Plotner's capture by Lansky.
Once this information inside the US government it was turned over to both the physicists and the new Big Pharma industry Titans controlled by the Rockefeller Foundation. Rockefeller chemists found out quickly that Pervitin behaves as an aggressive, synthetic shortcut that bypasses natural solar-photonic inputs to force a radical, short-term acceleration of local time flow. Since this was shared with both biologists and chemists melanin became a focus target of DARPA and the space program from 1950-1983 until the human genome project was begun.
What was the link between the drugs and mercury experiments?
Pervitin sounds is a drug that alters perception and energy density to influence time flow perception. This drug also seems to have some interesting links to the GLP1 A drugs because amphetamines are found to lead to increase excess CLIP peptide fragments that floods the circulatory system, travels to the hypothalamus, and blocks the native satiety pathways. Concurrently, it welds the HCO3- vagal exhaust pipe shut at the pancreatic interface. The body can no longer flush out its heavy deuterium grease, inducing structural Lattice Lock and causing the profound post-stimulant crashes, rampant internal inflammation, and eventual insulin resistance that was documented by Rockefeller chemists in chronic wartime users (including Adolf Hitler himself, who received daily, multi-drug injections from Dr. Theodor Morell.
My decentralized thesis exposes the multi-generational, synthetic mechanism linking the Wehrmacht’s amphetamine (Pervitin) to modern Big Pharma’s blockbuster GLP-1 agonists (Ozempic/Wegovy/Mounjaro). Both chemical interventions bypass natural solar-photonic and magnetic inputs to forcefully alter localized energy density and manipulate time-flow perception within the neural and gut-vagal architectures.
By looking through my decentralized framework, you can see that modern GLP-1 agonists are the direct spiritual and thermodynamic successors to Pervitin. They are both high-entropy biological short-term hacks designed to manipulate the satiety volume knob while leaving behind an un-cleared tailpipe of deuterium grease.
The Nazi's were trying to use amphetamines and mercury to engineer a customizable space-time bubble where the internal clock (time flow meter) slowed down to such an extent that the surrounding universe would move rapidly around it. It was an active mechanism to preserve knowledge, shield materials from entropic decay, or manipulate gravitational push gradients (effective propulsion for space) by bending the un-bound magnetic-field around a heavy ceramic shell.
The historical records regarding Die Glocke’s early testing reveal its catastrophic, unshielded physical feedback loop on nearby organic matter: within its active field, plants decomposed into a grease, blood gelled, and animal tissues grew crystallization structures, killing multiple early researchers.
The ancients at Teotihuacan and China understood the immense, volatile power of the fluidic mercury vortex. They handled it with the master patience of blacksmiths, leaving it in vast, quiet, un-moving subterranean lakes beneath titanic stone capacitors to safely buffer their civilizations from space-time excursions. When the SS found about the ancients they took up the physics and some of this infomation was slipped from SS Surgeon Kurt Plotner to Meyer Lansky and then to General Groves. It became part of the MKULTRA early portfolio.
Plotner told Groves the Nazis were trying to bypass the native stage of nature, attempted to force the magnetic-field into submission using brute-force mechanics and artificial voltage. This info stunned Groves and he went straight to the Dulles harvested pre-Paperclip physicists to run this by them who were in the Manhattan Project. The Nazi's successfully proved that energy density directly dictates the flow of time, but they paid the ultimate thermodynamic bill because they didn't respect the delicate, high-dielectric liquid stage that biological life requires to survive the torque of the cosmos.
DISSCUSSION
Pervitin was the Chemical Nazi Hammer the Rockefeller dynasty got from Lansky and Groves: The drug was studied in MKULTRA and it forces an explosive, unnatural dump of dopamine and norepinephrine. This artificially spikes the cell's short-term energy density profile, compressing experienced time. To the soldier or user, time slows down perceptually, fatigue vanishes, and hunger is deleted.
GLP-1 Agonists became the Rockefeller Continuous Mimic of the NAzi science: Modern GLP-1 analogues (semaglutide, tirzepatide, retatrude) chemically manipulate the same brain-gut axis. By mimicking the native glucagon-like peptide-1, they force the stomach to slow its gastric emptying rate, physically magnetically freezing food in the gut. To the enteric nervous system, this physical standstill acts as a localized time-dilation event. The vagal signals to the brain signal a perpetual state of "fullness" because the internal mechanical clock of digestion has been dragged to a near-halt.
The core problem with both interventions, GP1-A and Hg, is that they extract energy and force a time-shift without fixing the dielectric stage (k= 160\))or cleaning the water table. This triggers the identical biochemical liquidation sequence in both cases.
Now you can see why the discovery of leptin was a watershed moment for Rockefeller University and their Foundation in 1994. When these synthetic molecules saturate the hypothalamus, they burn out the native PC1/3 and PC2 pro-hormone convertase pathways. Because the cells are operating under isolated indoor blue light or electronic fields without the protective triplet-state oxygen, the POMC pro-hormone spine is cleaved incorrectly into synthetic peptides. This is where the GLP1A idea emerged from MKULTRA.
Instead of producing clean, fat-burning alpha-MSH, the system floods the circulatory matrix with an excess of CLIP (Corticotropin-like Intermediate Peptide) fragments.
The Hypothalamic Blockade: This tidal wave of CLIP travels straight back to the arcuate nucleus, competitively binding and blocking the native melanocortin-4 receptors (MC4R).
The Rebound Explosion: This is precisely why when a patient discontinues a GLP-1 drug or an amphetamine, they suffer from hyperphagia (uncontrollable, frantic food noise and hunger cravings). The synthetic hack leaves their brain completely blinded by a backup of CLIP, demanding massive caloric infusions to try and overcome the localized energy deficit.
The underground, massive "research chemical" scale-testing of Retatrutide (Reta) before its formal FDA approval is a historic manifestation of decentralized deuterated populations hacking their own biology because they are experiencing the side effects of a magnetic excursion without knowing about it. Driven by a collective desire to bypass institutional gatekeepers, labs and decentralized biohackers, they are testing this triple-agonist molecule at an unprecedented, global scale for the Rockefeller dynasty to taper the Ponzi scheme.
While first-generation semaglutide (Wegovy) targets a single hormone pathway (GLP-1), and second-generation tirzepatide (Mounjaro) targets two (GLP-1 + GIP), Retatrutide is a "Triple-G" agonist, simultaneously stimulating GLP-1, GIP, and Glucagon receptors. The addition of the glucagon receptor pathway is what makes Reta behave completely differently in biohacking labs. Glucagon directly forces the liver and adipocytes to dump stored energy. It turns up the heat by accelerating mitochondrial output, matching the explosive 28% average weight loss documented in recent Phase 3 TRIUMPH-1 trials.
By forcing three distinct metabolic pathways to fire simultaneously, Reta dramatically drives up the ordered appearance of energy expenditure. It tricks the biological system into a massive time-dilation state. The hypothalamic feeding centers are completely blinded to physical reality, deleting "food noise" entirely because the internal clock of energetic signaling has been cranked to absolute maximum velocity.
WHY RETA WILL DESTROY HUMANS?
It is the ultimate MKULTRA drug. It causes a change in perception and time and you will be fooled into causing your own death under the guise of helath optimization. The reason the global grey-market testing of Reta is a monumental gamble is because it forces an extreme energetic extraction from the cell without correcting the underlying dielectric stage (k = 160) or purging the environmental deuterium grease
By running a triple-engine on a collapsed, bulk-water matrix (k = 78), the long-term thermodynamic bill is compounded: HOW?
Because these peptides are used by a population constantly bathed in isolated artificial blue light and chronic non-native EMF (nnEMF), during an active magnetic excursion, the local oxygen states are heavily skewed into volatile singlet oxygen.
The pro-hormone convertase enzymes (PC1/3 and PC2) are structurally blinded by this spin-noise. When users inevitably cycle off or exhaust their grey-market Reta supplies, their broken POMC engines will experience a catastrophic backup, cleaving the alpha-helical spine into a massive, unprecedented flood of Corticotropin-like Intermediate Peptide (CLIP) fragments.
Users will get the Nazi ending.
Once the synthetic triple-agonist signal is dropped and the hypothalamus is saturated with an excess of CLIP fragments, the system triggers the identical Lattice Lock collapse seen in chronic Pervitin users, but amplified by the triple-receptor debt:The Hyperphagia Spike: The excess CLIP completely blocks the native melanocortin receptors (MC4R), inducing a state of frantic, uncontrollable metabolic hunger.
Welding the Vagal Tailpipe: The CLIP blockade de-energizes the bicarbonate (HCO3-) vagal exhaust system at the pancreatic interface. Carbonic anhydrase loses its quantum spin-alignment. The biological tailpipe is welded shut.
The Mass Crash: The heavy deuterium grease and tritium mass accumulated from a modern bulk-water diet during an excursion has nowhere to go. It backs up straight into the pancreatic beta cells, permanently jamming the ATP synthase rotors and forcing an immediate, systemic Landauer liquidation, yielding rampant internal tissue inflammation, rapid regain of weight purely as high-viscosity fat mass, and structural insulin resistance.
The Universal Invariance
The current peptide craze is a grand planetary experiment in trying to force the biological network into compliance using synthetic, isolated chemical signals. It mirrors the exact mistake the SS made with high-speed counter-rotating mercury barrels or the 1940s Rockefeller chemists made with Pervitin: extracting short-term time flow advantages while completely ignoring the degradation of the material dielectric stage.
Noether’s theorem dictates that the total energy cannot be cheated.
If you use Reta to force a massive structural reorganization of mass without deploying the natural boundary conditions, like paramagnetic volcanic anchors, chiral copper loops, high-dielectric phycocyanin buffers, and the natural light-dark template of nature, the system will eventually execute its own harsh, thermodynamic audit. The symphony always re-establishes its baseline frequency.
SUMMARY
The Rockefeller NAZI MKULTRA Legacy: Tracking the Multi-Drug Injections first done by the CIA at Camp King by Walter Scheiber in Project Bluebird was merged with MKULTRA in West Germany. I found all of this information in the boxes at Charity Hospital.
The records of Dr. Theodor Morell’s daily injections into Adolf Hitler reveal a cocktails of Pervitin, glucose infusions, and animal organ extracts. The Rockefeller-trained chemists of the mid-20th century watched this clinical experiment in real-time. They documented that the combination of high-sugar infusions (loading the matrix with deuterium) alongside a drug that forced an artificial time-dilation (Pervitin) accelerated the tissue's physical decay.
They saw a man who was hired by the Rothschild's/Vatican/Crown to Transfer Europe's Jews to Rothschild's Palestine inherited from the Treaty of Versailee and he began his task with immense energy density and rapidly degenerate into an un-coordinated, trembling, prematurely aged system. His biological base oscillators had been driven into absolute Lattice Lock by the clogging of his vagal exhaust with heavy hydrogne isotopes.
Modern medicine has re-packaged this exact 1940s Rockefeller-Morell protocol into a weekly self-injection pen. It provides a short-term, abstract illusion of metabolic efficiency while systematically welding the body's physical tailpipe shut, ensuring an eventual systemic crash when the un-cleared deuterium mass finally shatters the local water table.
CITES
x.com/DrJackKruse/st…
The Nazis weren't inventing a new physics; they were attempting to mechanize and compress the passive macroscopic space-time regulation methods of the ancients into a mobile, high-voltage active antigravity device. A lot of this data made it through Operation Paperclip, NASA, DARPA, and into the space program.
The Ancient Method (Teotihuacan & China): They used vast, static quantities of liquid mercury laid out in subterranean river paths under heavy geometric capacitors. They relied on mercury's natural relativistic electronic density and raw volume mass (13.53g/cm^3) to passively pin magnetic flux and hold local space-time order.
The SS realized they could bypass the need to build a literal pyramid or dig a massive lake by introducing macroscopic rotational spin-quanta. By taking a mercury-based liquid (Xerum 525) and forcing it through two counter-rotating cylinders at hyper-high RPMs under extreme high-voltage electrical excitation, they artificially multiplied the local energy density vector by orders of magnitude.
By spinning the mercury in opposing directions, they achieved Common Mode Rejection. The transverse components of the massive electromagnetic currents crashed directly into one another and nullified. This forced a massive centripetal wave implosion, compressing the local magnetic-field into an intensely focused, longitudinal column.
The strategic goal of Die Glocke under Hans Kammler was not simply to make a weapon, but to construct a Timeline Disruptor and Reality Anchor. By driving the ordered component of local energy density to structural extremes inside the Bell, they aimed to completely decouple the interior chamber from the background planetary time-flow. They knew about the ancient megalith sites use of physics to do the same during excursions. I found evidence of this in the MKULTRA boxes in Charity Hospital.
Why was the link made?
Plotner told Groves about the use of amphetamines in the SS to Groves. He relayed it was done to mind control soldiers to better performance and the process began and was field tested in the 1939 Olympics. Big Harma complany Temmler patented and launched Pervitin in 1938 after studying Mexican peyote, and through an alliance with the Wehrmacht and the SS high command, they supplied tens of millions of tablets to fuel atheletes and soldiers in WW2 to power the mind to perform under sleepless, to facilitate the high-velocity campaigns of the Blitzkrieg.
What did the Nazi Plotner relay to Groves via Lansky? Through the lens of my decentralized thesis, the pharmacology of Pervitin reveals a profound, synthetic hijacking of the body's peripheral POMC clipping architecture and energy-density regulators. This was how the SCN melanin RPE became a target of the Nazi's. They realized melanin was paramagnetic and it was chiral and it was dram to magnetic fields. These Hg experiments and the link to melanin was made by Plotner's capture by Lansky.
Once this information inside the US government it was turned over to both the physicists and the new Big Pharma industry Titans controlled by the Rockefeller Foundation. Rockefeller chemists found out quickly that Pervitin behaves as an aggressive, synthetic shortcut that bypasses natural solar-photonic inputs to force a radical, short-term acceleration of local time flow. Since this was shared with both biologists and chemists melanin became a focus target of DARPA and the space program from 1950-1983 until the human genome project was begun.
What was the link between the drugs and mercury experiments?
Pervitin sounds is a drug that alters perception and energy density to influence time flow perception. This drug also seems to have some interesting links to the GLP1 A drugs because amphetamines are found to lead to increase excess CLIP peptide fragments that floods the circulatory system, travels to the hypothalamus, and blocks the native satiety pathways. Concurrently, it welds the HCO3- vagal exhaust pipe shut at the pancreatic interface. The body can no longer flush out its heavy deuterium grease, inducing structural Lattice Lock and causing the profound post-stimulant crashes, rampant internal inflammation, and eventual insulin resistance that was documented by Rockefeller chemists in chronic wartime users (including Adolf Hitler himself, who received daily, multi-drug injections from Dr. Theodor Morell.
My decentralized thesis exposes the multi-generational, synthetic mechanism linking the Wehrmacht’s amphetamine (Pervitin) to modern Big Pharma’s blockbuster GLP-1 agonists (Ozempic/Wegovy/Mounjaro). Both chemical interventions bypass natural solar-photonic and magnetic inputs to forcefully alter localized energy density and manipulate time-flow perception within the neural and gut-vagal architectures.
By looking through my decentralized framework, you can see that modern GLP-1 agonists are the direct spiritual and thermodynamic successors to Pervitin. They are both high-entropy biological short-term hacks designed to manipulate the satiety volume knob while leaving behind an un-cleared tailpipe of deuterium grease.
The Nazi's were trying to use amphetamines and mercury to engineer a customizable space-time bubble where the internal clock (time flow meter) slowed down to such an extent that the surrounding universe would move rapidly around it. It was an active mechanism to preserve knowledge, shield materials from entropic decay, or manipulate gravitational push gradients (effective propulsion for space) by bending the un-bound magnetic-field around a heavy ceramic shell.
The historical records regarding Die Glocke’s early testing reveal its catastrophic, unshielded physical feedback loop on nearby organic matter: within its active field, plants decomposed into a grease, blood gelled, and animal tissues grew crystallization structures, killing multiple early researchers.
The ancients at Teotihuacan and China understood the immense, volatile power of the fluidic mercury vortex. They handled it with the master patience of blacksmiths, leaving it in vast, quiet, un-moving subterranean lakes beneath titanic stone capacitors to safely buffer their civilizations from space-time excursions. When the SS found about the ancients they took up the physics and some of this infomation was slipped from SS Surgeon Kurt Plotner to Meyer Lansky and then to General Groves. It became part of the MKULTRA early portfolio.
Plotner told Groves the Nazis were trying to bypass the native stage of nature, attempted to force the magnetic-field into submission using brute-force mechanics and artificial voltage. This info stunned Groves and he went straight to the Dulles harvested pre-Paperclip physicists to run this by them who were in the Manhattan Project. The Nazi's successfully proved that energy density directly dictates the flow of time, but they paid the ultimate thermodynamic bill because they didn't respect the delicate, high-dielectric liquid stage that biological life requires to survive the torque of the cosmos.
DISSCUSSION
Pervitin was the Chemical Nazi Hammer the Rockefeller dynasty got from Lansky and Groves: The drug was studied in MKULTRA and it forces an explosive, unnatural dump of dopamine and norepinephrine. This artificially spikes the cell's short-term energy density profile, compressing experienced time. To the soldier or user, time slows down perceptually, fatigue vanishes, and hunger is deleted.
GLP-1 Agonists became the Rockefeller Continuous Mimic of the NAzi science: Modern GLP-1 analogues (semaglutide, tirzepatide, retatrude) chemically manipulate the same brain-gut axis. By mimicking the native glucagon-like peptide-1, they force the stomach to slow its gastric emptying rate, physically magnetically freezing food in the gut. To the enteric nervous system, this physical standstill acts as a localized time-dilation event. The vagal signals to the brain signal a perpetual state of "fullness" because the internal mechanical clock of digestion has been dragged to a near-halt.
The core problem with both interventions, GP1-A and Hg, is that they extract energy and force a time-shift without fixing the dielectric stage (k= 160\))or cleaning the water table. This triggers the identical biochemical liquidation sequence in both cases.
Now you can see why the discovery of leptin was a watershed moment for Rockefeller University and their Foundation in 1994. When these synthetic molecules saturate the hypothalamus, they burn out the native PC1/3 and PC2 pro-hormone convertase pathways. Because the cells are operating under isolated indoor blue light or electronic fields without the protective triplet-state oxygen, the POMC pro-hormone spine is cleaved incorrectly into synthetic peptides. This is where the GLP1A idea emerged from MKULTRA.
Instead of producing clean, fat-burning alpha-MSH, the system floods the circulatory matrix with an excess of CLIP (Corticotropin-like Intermediate Peptide) fragments.
The Hypothalamic Blockade: This tidal wave of CLIP travels straight back to the arcuate nucleus, competitively binding and blocking the native melanocortin-4 receptors (MC4R).
The Rebound Explosion: This is precisely why when a patient discontinues a GLP-1 drug or an amphetamine, they suffer from hyperphagia (uncontrollable, frantic food noise and hunger cravings). The synthetic hack leaves their brain completely blinded by a backup of CLIP, demanding massive caloric infusions to try and overcome the localized energy deficit.
The underground, massive "research chemical" scale-testing of Retatrutide (Reta) before its formal FDA approval is a historic manifestation of decentralized deuterated populations hacking their own biology because they are experiencing the side effects of a magnetic excursion without knowing about it. Driven by a collective desire to bypass institutional gatekeepers, labs and decentralized biohackers, they are testing this triple-agonist molecule at an unprecedented, global scale for the Rockefeller dynasty to taper the Ponzi scheme.
While first-generation semaglutide (Wegovy) targets a single hormone pathway (GLP-1), and second-generation tirzepatide (Mounjaro) targets two (GLP-1 + GIP), Retatrutide is a "Triple-G" agonist, simultaneously stimulating GLP-1, GIP, and Glucagon receptors. The addition of the glucagon receptor pathway is what makes Reta behave completely differently in biohacking labs. Glucagon directly forces the liver and adipocytes to dump stored energy. It turns up the heat by accelerating mitochondrial output, matching the explosive 28% average weight loss documented in recent Phase 3 TRIUMPH-1 trials.
By forcing three distinct metabolic pathways to fire simultaneously, Reta dramatically drives up the ordered appearance of energy expenditure. It tricks the biological system into a massive time-dilation state. The hypothalamic feeding centers are completely blinded to physical reality, deleting "food noise" entirely because the internal clock of energetic signaling has been cranked to absolute maximum velocity.
WHY RETA WILL DESTROY HUMANS?
It is the ultimate MKULTRA drug. It causes a change in perception and time and you will be fooled into causing your own death under the guise of helath optimization. The reason the global grey-market testing of Reta is a monumental gamble is because it forces an extreme energetic extraction from the cell without correcting the underlying dielectric stage (k = 160) or purging the environmental deuterium grease
By running a triple-engine on a collapsed, bulk-water matrix (k = 78), the long-term thermodynamic bill is compounded: HOW?
Because these peptides are used by a population constantly bathed in isolated artificial blue light and chronic non-native EMF (nnEMF), during an active magnetic excursion, the local oxygen states are heavily skewed into volatile singlet oxygen.
The pro-hormone convertase enzymes (PC1/3 and PC2) are structurally blinded by this spin-noise. When users inevitably cycle off or exhaust their grey-market Reta supplies, their broken POMC engines will experience a catastrophic backup, cleaving the alpha-helical spine into a massive, unprecedented flood of Corticotropin-like Intermediate Peptide (CLIP) fragments.
Users will get the Nazi ending.
Once the synthetic triple-agonist signal is dropped and the hypothalamus is saturated with an excess of CLIP fragments, the system triggers the identical Lattice Lock collapse seen in chronic Pervitin users, but amplified by the triple-receptor debt:The Hyperphagia Spike: The excess CLIP completely blocks the native melanocortin receptors (MC4R), inducing a state of frantic, uncontrollable metabolic hunger.
Welding the Vagal Tailpipe: The CLIP blockade de-energizes the bicarbonate (HCO3-) vagal exhaust system at the pancreatic interface. Carbonic anhydrase loses its quantum spin-alignment. The biological tailpipe is welded shut.
The Mass Crash: The heavy deuterium grease and tritium mass accumulated from a modern bulk-water diet during an excursion has nowhere to go. It backs up straight into the pancreatic beta cells, permanently jamming the ATP synthase rotors and forcing an immediate, systemic Landauer liquidation, yielding rampant internal tissue inflammation, rapid regain of weight purely as high-viscosity fat mass, and structural insulin resistance.
The Universal Invariance
The current peptide craze is a grand planetary experiment in trying to force the biological network into compliance using synthetic, isolated chemical signals. It mirrors the exact mistake the SS made with high-speed counter-rotating mercury barrels or the 1940s Rockefeller chemists made with Pervitin: extracting short-term time flow advantages while completely ignoring the degradation of the material dielectric stage.
Noether’s theorem dictates that the total energy cannot be cheated.
If you use Reta to force a massive structural reorganization of mass without deploying the natural boundary conditions, like paramagnetic volcanic anchors, chiral copper loops, high-dielectric phycocyanin buffers, and the natural light-dark template of nature, the system will eventually execute its own harsh, thermodynamic audit. The symphony always re-establishes its baseline frequency.
SUMMARY
The Rockefeller NAZI MKULTRA Legacy: Tracking the Multi-Drug Injections first done by the CIA at Camp King by Walter Scheiber in Project Bluebird was merged with MKULTRA in West Germany. I found all of this information in the boxes at Charity Hospital.
The records of Dr. Theodor Morell’s daily injections into Adolf Hitler reveal a cocktails of Pervitin, glucose infusions, and animal organ extracts. The Rockefeller-trained chemists of the mid-20th century watched this clinical experiment in real-time. They documented that the combination of high-sugar infusions (loading the matrix with deuterium) alongside a drug that forced an artificial time-dilation (Pervitin) accelerated the tissue's physical decay.
They saw a man who was hired by the Rothschild's/Vatican/Crown to Transfer Europe's Jews to Rothschild's Palestine inherited from the Treaty of Versailee and he began his task with immense energy density and rapidly degenerate into an un-coordinated, trembling, prematurely aged system. His biological base oscillators had been driven into absolute Lattice Lock by the clogging of his vagal exhaust with heavy hydrogne isotopes.
Modern medicine has re-packaged this exact 1940s Rockefeller-Morell protocol into a weekly self-injection pen. It provides a short-term, abstract illusion of metabolic efficiency while systematically welding the body's physical tailpipe shut, ensuring an eventual systemic crash when the un-cleared deuterium mass finally shatters the local water table.
CITES
x.com/DrJackKruse/st…
5. Next slide.
6. The animal kingdom understands the biophysics of skin atrophy implicitly. A mate is selected based on the vibrant, high-redox coloring of their solar callus, whether it is the bright red chest of a gelada baboon, the iridescent feathers of a bird, or the flush of a healthy, sun-charged human skin matrix. Nature rewards ordered energy density and high dielectric power.
The Mponeng "ghost miners" proved what happens when you remove light from the three pillars of biology. Modern human civilization, by hiding behind window glass, sunscreen, sunglasses, and synthetic peptide injections, has turned entire continents into subterranean gold mines, creating a generation of pale, atrophied, CLIP-saturated electrical resistors who have traded their planetary magnetic sovereignty for a temporary, fragile chemical illusion.
Maybe now you know why I gave you a Godwit blog now on Patreon?
The Godwit story explains what BigHarma is attempting to do to humanity during this excursion. Being pale can happen many ways, and it is not a sign of wellness contrary to popular dermatologic speeches.
Being pale = the largest organ in your body has atrophied for some reason. It could be a mine, an excursion, or a drug behind it. Even animals besides humans use their solar callus to draw mates.Folks who spend time in the sun can change their surface color by assimilating certain frequencies of sunlight to take red tones because IR-A light increases our RBC's production when our skin is hit with sunlight it undergoes dermal pooling to make our skin flush with blood. When the sun has powerful UV light shining on our skin and eyes (latitude-based), more triplet oxygen is found in our blood changing its color to a deep red due to the increased amount of oxygen in it. When the dynamo weakens singlet oxygen shows up and the blood is not as red.
There are many interesting stories from Lavoisier about surgeons doing blood letting from equatorial crossing where doctors thought they hit arteries because the color of the blood changed from the higher latitudes. From a biological/anthropological perspective, this color change signals health and vitality and high redox potential to members of our species who see us in nature. The use of sunscreen and sunglasses is the most common form of modern skin atrophy in humans. It isn't mining any longer. Soon Reta might be the number one cause.
Antoine Lavoisier’s historical accounts of equatorial ship surgeons panic-striking when performing bloodlettings are perfectly explained by my framework. The doctors thought they had accidentally punctured an artery because the venous blood was a shocking, brilliant scarlet color.
Centralized biology chalks this up to abstract temperature-regulated vasodilation.
The true biophysical mechanism is Photonic Dermal Pooling and Spin-Wave Polarization:
1. When your skin is hit with natural, full-spectrum equatorial light, the intense infrared (IR-A) frequencies penetrate deep into the tissue, stimulating mitochondrial cytochrome c oxidase and triggering a massive surge in red blood cell (RBC) production. The skin coordinates dermal pooling, intentionally drawing the blood volume to the surface to act as a liquid-crystalline antenna.
2. The Triplet Invariance: Under high-latitude or equatorial solar flux, the highly organized electromagnetic environment forces blood oxygen to lock into its stable, ground-state triplet oxygen configuration. This high-dielectric coherence changes the physical light-absorption properties of the hemoglobin molecule, turning the venous blood into a hyper-oxygenated, bright scarlet fluid that mirrors arterial blood. It is a direct, visible printout of maximum redox potential.
When a human enters a deep gold mine, undergoes a planetary magnetic excursion, or applies the modern chemical equivalent, sunglasses and chemical sunscreen, the planetary dynamo triplet oxygen link is broken. The skin does not just lose color; it undergoes a profound structural liquidation.The Sunglass Deception: When you wear sunglasses under the sun, you blind the central LC oscillator (the eye-pineal melanin axis). The brain registers a dark environment, failing to send the systemic signal to upregulate MITF (the master melanogenesis transcription pathway). The skin is left entirely unshielded.
The Singlet Rot: Without a melanin-and-copper semiconductor grid to execute common-mode rejection, incoming light cannot be cleanly routed. The system slips from its (1/137) grip. The local oxygen drops into volatile, excited singlet oxygen. This quantum spin noise disrupts the pro-hormone convertases in POMc and CLIP.
The Atrophy: The POMC pro-hormone spine is cleaved incorrectly, generating a massive, toxic dump of Corticotropin-like Intermediate Peptide (CLIP) while completely suppressing fat-burning, negentropic alpha-MSH. The water table loses its structured exclusion zones, viscosity spikes, and the skin turns grey, thin, and atrophied. The largest organ in the human body has been driven into Lattice Lock because its connection to the solar charger was deleted.
My prediction that Retatrutide (Reta) will soon become the number one cause of human skin atrophy is an inevitable mathematical certainty under the decentralized thesis you're reading right now on Patreon.
When research labs and biohackers scale-test triple-agonists like Reta under non-native artificial blue light and chronic nnEMF during a magnetic excursion, they are forcing a massive, hyper-accelerated extraction of mitochondrial energy density without fixing the underlying water dielectric stage (k = 78).
This massive, un-pruned thermodynamic debt burns out the native melanocortin pathways. The resulting catastrophic tidal wave of CLIP fragmentscompletely blocks the hypothalamic and peripheral MC4R satiety and pigmentation receptors.Melanogenesis stops completely.
The human body, starved of its natural, light-driven negentropic repair cycle, experiences an artificial, indoor "Carrington Event."
The user loses their solar callus, their skin atrophies and turns a bloodless, pale-grey color, and their vagal bicarbonate tailpipe is welded shut, locking them into a state of structural insulin resistance and deep biological decay the moment the synthetic chemical infusion stops. Their goal is to created the 1944 NAZI phenotype in the world to Taper the Ponzi scheme to help their banking and drug business. You are now informed.
CITES
patreon.com/posts/decentra…
The Mponeng "ghost miners" proved what happens when you remove light from the three pillars of biology. Modern human civilization, by hiding behind window glass, sunscreen, sunglasses, and synthetic peptide injections, has turned entire continents into subterranean gold mines, creating a generation of pale, atrophied, CLIP-saturated electrical resistors who have traded their planetary magnetic sovereignty for a temporary, fragile chemical illusion.
Maybe now you know why I gave you a Godwit blog now on Patreon?
The Godwit story explains what BigHarma is attempting to do to humanity during this excursion. Being pale can happen many ways, and it is not a sign of wellness contrary to popular dermatologic speeches.
Being pale = the largest organ in your body has atrophied for some reason. It could be a mine, an excursion, or a drug behind it. Even animals besides humans use their solar callus to draw mates.Folks who spend time in the sun can change their surface color by assimilating certain frequencies of sunlight to take red tones because IR-A light increases our RBC's production when our skin is hit with sunlight it undergoes dermal pooling to make our skin flush with blood. When the sun has powerful UV light shining on our skin and eyes (latitude-based), more triplet oxygen is found in our blood changing its color to a deep red due to the increased amount of oxygen in it. When the dynamo weakens singlet oxygen shows up and the blood is not as red.
There are many interesting stories from Lavoisier about surgeons doing blood letting from equatorial crossing where doctors thought they hit arteries because the color of the blood changed from the higher latitudes. From a biological/anthropological perspective, this color change signals health and vitality and high redox potential to members of our species who see us in nature. The use of sunscreen and sunglasses is the most common form of modern skin atrophy in humans. It isn't mining any longer. Soon Reta might be the number one cause.
Antoine Lavoisier’s historical accounts of equatorial ship surgeons panic-striking when performing bloodlettings are perfectly explained by my framework. The doctors thought they had accidentally punctured an artery because the venous blood was a shocking, brilliant scarlet color.
Centralized biology chalks this up to abstract temperature-regulated vasodilation.
The true biophysical mechanism is Photonic Dermal Pooling and Spin-Wave Polarization:
1. When your skin is hit with natural, full-spectrum equatorial light, the intense infrared (IR-A) frequencies penetrate deep into the tissue, stimulating mitochondrial cytochrome c oxidase and triggering a massive surge in red blood cell (RBC) production. The skin coordinates dermal pooling, intentionally drawing the blood volume to the surface to act as a liquid-crystalline antenna.
2. The Triplet Invariance: Under high-latitude or equatorial solar flux, the highly organized electromagnetic environment forces blood oxygen to lock into its stable, ground-state triplet oxygen configuration. This high-dielectric coherence changes the physical light-absorption properties of the hemoglobin molecule, turning the venous blood into a hyper-oxygenated, bright scarlet fluid that mirrors arterial blood. It is a direct, visible printout of maximum redox potential.
When a human enters a deep gold mine, undergoes a planetary magnetic excursion, or applies the modern chemical equivalent, sunglasses and chemical sunscreen, the planetary dynamo triplet oxygen link is broken. The skin does not just lose color; it undergoes a profound structural liquidation.The Sunglass Deception: When you wear sunglasses under the sun, you blind the central LC oscillator (the eye-pineal melanin axis). The brain registers a dark environment, failing to send the systemic signal to upregulate MITF (the master melanogenesis transcription pathway). The skin is left entirely unshielded.
The Singlet Rot: Without a melanin-and-copper semiconductor grid to execute common-mode rejection, incoming light cannot be cleanly routed. The system slips from its (1/137) grip. The local oxygen drops into volatile, excited singlet oxygen. This quantum spin noise disrupts the pro-hormone convertases in POMc and CLIP.
The Atrophy: The POMC pro-hormone spine is cleaved incorrectly, generating a massive, toxic dump of Corticotropin-like Intermediate Peptide (CLIP) while completely suppressing fat-burning, negentropic alpha-MSH. The water table loses its structured exclusion zones, viscosity spikes, and the skin turns grey, thin, and atrophied. The largest organ in the human body has been driven into Lattice Lock because its connection to the solar charger was deleted.
My prediction that Retatrutide (Reta) will soon become the number one cause of human skin atrophy is an inevitable mathematical certainty under the decentralized thesis you're reading right now on Patreon.
When research labs and biohackers scale-test triple-agonists like Reta under non-native artificial blue light and chronic nnEMF during a magnetic excursion, they are forcing a massive, hyper-accelerated extraction of mitochondrial energy density without fixing the underlying water dielectric stage (k = 78).
This massive, un-pruned thermodynamic debt burns out the native melanocortin pathways. The resulting catastrophic tidal wave of CLIP fragmentscompletely blocks the hypothalamic and peripheral MC4R satiety and pigmentation receptors.Melanogenesis stops completely.
The human body, starved of its natural, light-driven negentropic repair cycle, experiences an artificial, indoor "Carrington Event."
The user loses their solar callus, their skin atrophies and turns a bloodless, pale-grey color, and their vagal bicarbonate tailpipe is welded shut, locking them into a state of structural insulin resistance and deep biological decay the moment the synthetic chemical infusion stops. Their goal is to created the 1944 NAZI phenotype in the world to Taper the Ponzi scheme to help their banking and drug business. You are now informed.
CITES
patreon.com/posts/decentra…
7. Every person that pushes peptides will have a Landauer liquidation of the skin, teeth, and RPE. The doctors and influencers peddling the Nazi drugs will all show the signs. Look for them because they will use methods to cover it up now that I am exposing them.
The Godwit survives its 11,000-kilometer journey because it follows the immutable laws of the planetary magnetic)-field. If humans continue to choose isolated chemical hacks while living as pale, atrophied "ghost miners" inside electronic cages, the thermodynamic debt will always finalize its audit. The symphony rewards the preservation of ordered energy density, matter must be structured before the clock can be safely turned.Humans do not have the Godwit pecten oculi to bail them out from "RETA" burnout.
Bringing the Bar-tailed Godwit (Limosa lapponica) and its pecten oculi into the architecture exposes the absolute evolutionary chasm between a master quantum traveler and a modern human trying to cheat the system with synthetic triple-agonists like Retatrutide (Reta)
The NAZI's MKULTRA program was built to create an Aryan Soldier who was Godwit like. You might have missed that point if you aren't reading my work.
The Godwit holds the record for the longest non-stop flight on Earth, flying over 11,000 to 13,000 kilometers from Alaska to New Zealand without eating, drinking, or resting. It doubles its body mass, packing away an immense concentration of fat, yet it suffers zero metabolic burnout, zero insulin resistance, and zero "Lattice Lock."
It can handle this radical energetic overload because its entire sensory system is anchored to a pristine, natural quantum-magnetic compass. Humans lack the specialized anatomy, specifically the pecten oculi and the highly concentrated Cry4 cryptochrome cone matrix, needed to safely buffer the massive time-dilation and energy-density shifts of a triple-agonist surge.
The bird's eye features a highly vascular, comb-like structure called the pecten oculi. While centralized biology claims its only function is to supply nutrition to the avascular retina, through my decentralized physics framework, the pecten serves a much higher thermodynamic purpose: it acts as a localized magnetic shield, a fluid homopolar regulator, and a heat-and-spin stabilizer.The Triplet Shield: As the Godwit undergoes its massive energetic burn across the unshielded sky, its pecten oculi and ultraviolet-sensitive cones utilize Cry4 cryptochromes to directly observe the Earth's geomagnetic field lines. When blue/UV light strikes this matrix, it triggers a radical pair mechanism, the biological manifestation of Chirality-Induced Spin Selectivity (CISS).
Preventing the Dumpster Fire: This continuous quantum-magnetic feedback loop ensures that the intense radiation from the high-altitude sun cannot force local tissue oxygen into volatile singlet states. The oxygen stays locked in its stable triplet ground state to keep the melanin in the pecten operational and getting rid of D+ as it flies.
Perfect POMC Splitting: Supported by this pristine magnetic template, the bird's pro-hormone convertase enzymes cleave the POMC spine with flawless precision. It produces a massive, clean stream of fat-burning alpha-MSH to fuel its flight muscles while completely suppressing toxic, insulin-resistant CLIP fragments. The bird can burn through its entire fat mass because its water table maintains a perfect, low-viscosity (k = 160)baseline. It never drops its electromagnetic grip (alpha = 1/137).
The Human Reta Burnout: Blown Out Engines Without a Shield
When a modern human injects Reta, they are demanding that their cells replicate the Godwit’s extreme fat-burning, liver-dumping metabolic overdrive. However, because humans are completely devoid of a pecten oculi or a highly active, light-driven Cry4 magnetic compass, the system has no way to phase-lock its internal fluids during the surge.
The user applies a triple-receptor chemical hammer while sitting in a low-ordered energy density desert, bathed in artificial screen light, disconnected from the earth, during an excursion, while slathered in chemical sunscreens that artificially induce skin atrophy.The Unbuffered Spin Noise: Without the Godwit's radical-pair filtering mechanism, the high-velocity mitochondrial rotation under Reta rapidly exhausts the local triplet oxygen pool. The intracellular stage collapses into a runaway singlet oxygen fire.
The CLIP Deluge: The enzymatic cutters (PC1/3 and PC2) lose their spin-alignment in the chaotic, bulk-water medium (k= 78). They make the errant cut along the pro-hormone spine, flooding the system with a massive wave of Corticotropin-like Intermediate Peptide (CLIP).
Welding the Exhaust Pipe: This tidal wave of CLIP blocks the native MC4R satiety pathways and completely de-energizes the bicarbonate vagal exhaust pipe at the pancreatic interface. The heavy, un-pruned deuterium grease from a modern lifestyle has nowhere to go. It backs up directly into the pancreatic beta cells, permanently jamming the ATP synthase rotors and forcing an eventual, catastrophic Landauer liquidation, yielding rapid regain of high-viscosity fat mass, thyroid C-cell risks, and structural insulin burnout.
The lesson of the Bar-tailed Godwit is absolute: you cannot safely alter metabolic time flow or handle massive energy conversions without an active, material dielectric shield to ground the spin noise. Humans using RETA cannot grow a pecten oculi, but through the direct application of decentralized physics, we can manually build its functional equivalent.
If a modern human is navigating a changing environment or using targeted peptides, they must deploy the macro-scale boundary conditions that centralized medicine ignores:Rebuilding the Melanin Grid: Throwing away the sunglasses and chemical sunscreens to allow natural, latitude-based full-spectrum light to initiate dermal pooling, restoring triplet-state oxygen and charging the water table back to (k = 160).
Mechanical Common-Mode Rejection: Wearing a Spurling chiral neck loop precisely over the vagal and carotid choke points to filter out transverse field noise, creating an active longitudinal scalar column that assists the body in clearing deuterium grease from the brain-gut axis.
The High-Dielectric Buffer: Utilizing Sunlight and my cold thermogenesis protocol while being grounded to paramagnetic basalt soil dressings to manually clear the bicarbonate exhaust pipe, preventing the anomalous volume isotope expansion that forces cells to swell like CME-stressed ice cubes. The phsyics scales from ice cubes to you.
The Godwit survives its 11,000-kilometer journey because it follows the immutable laws of the planetary magnetic)-field. If humans continue to choose isolated chemical hacks while living as pale, atrophied "ghost miners" inside electronic cages, the thermodynamic debt will always finalize its audit. The symphony rewards the preservation of ordered energy density, matter must be structured before the clock can be safely turned.Humans do not have the Godwit pecten oculi to bail them out from "RETA" burnout.
Bringing the Bar-tailed Godwit (Limosa lapponica) and its pecten oculi into the architecture exposes the absolute evolutionary chasm between a master quantum traveler and a modern human trying to cheat the system with synthetic triple-agonists like Retatrutide (Reta)
The NAZI's MKULTRA program was built to create an Aryan Soldier who was Godwit like. You might have missed that point if you aren't reading my work.
The Godwit holds the record for the longest non-stop flight on Earth, flying over 11,000 to 13,000 kilometers from Alaska to New Zealand without eating, drinking, or resting. It doubles its body mass, packing away an immense concentration of fat, yet it suffers zero metabolic burnout, zero insulin resistance, and zero "Lattice Lock."
It can handle this radical energetic overload because its entire sensory system is anchored to a pristine, natural quantum-magnetic compass. Humans lack the specialized anatomy, specifically the pecten oculi and the highly concentrated Cry4 cryptochrome cone matrix, needed to safely buffer the massive time-dilation and energy-density shifts of a triple-agonist surge.
The bird's eye features a highly vascular, comb-like structure called the pecten oculi. While centralized biology claims its only function is to supply nutrition to the avascular retina, through my decentralized physics framework, the pecten serves a much higher thermodynamic purpose: it acts as a localized magnetic shield, a fluid homopolar regulator, and a heat-and-spin stabilizer.The Triplet Shield: As the Godwit undergoes its massive energetic burn across the unshielded sky, its pecten oculi and ultraviolet-sensitive cones utilize Cry4 cryptochromes to directly observe the Earth's geomagnetic field lines. When blue/UV light strikes this matrix, it triggers a radical pair mechanism, the biological manifestation of Chirality-Induced Spin Selectivity (CISS).
Preventing the Dumpster Fire: This continuous quantum-magnetic feedback loop ensures that the intense radiation from the high-altitude sun cannot force local tissue oxygen into volatile singlet states. The oxygen stays locked in its stable triplet ground state to keep the melanin in the pecten operational and getting rid of D+ as it flies.
Perfect POMC Splitting: Supported by this pristine magnetic template, the bird's pro-hormone convertase enzymes cleave the POMC spine with flawless precision. It produces a massive, clean stream of fat-burning alpha-MSH to fuel its flight muscles while completely suppressing toxic, insulin-resistant CLIP fragments. The bird can burn through its entire fat mass because its water table maintains a perfect, low-viscosity (k = 160)baseline. It never drops its electromagnetic grip (alpha = 1/137).
The Human Reta Burnout: Blown Out Engines Without a Shield
When a modern human injects Reta, they are demanding that their cells replicate the Godwit’s extreme fat-burning, liver-dumping metabolic overdrive. However, because humans are completely devoid of a pecten oculi or a highly active, light-driven Cry4 magnetic compass, the system has no way to phase-lock its internal fluids during the surge.
The user applies a triple-receptor chemical hammer while sitting in a low-ordered energy density desert, bathed in artificial screen light, disconnected from the earth, during an excursion, while slathered in chemical sunscreens that artificially induce skin atrophy.The Unbuffered Spin Noise: Without the Godwit's radical-pair filtering mechanism, the high-velocity mitochondrial rotation under Reta rapidly exhausts the local triplet oxygen pool. The intracellular stage collapses into a runaway singlet oxygen fire.
The CLIP Deluge: The enzymatic cutters (PC1/3 and PC2) lose their spin-alignment in the chaotic, bulk-water medium (k= 78). They make the errant cut along the pro-hormone spine, flooding the system with a massive wave of Corticotropin-like Intermediate Peptide (CLIP).
Welding the Exhaust Pipe: This tidal wave of CLIP blocks the native MC4R satiety pathways and completely de-energizes the bicarbonate vagal exhaust pipe at the pancreatic interface. The heavy, un-pruned deuterium grease from a modern lifestyle has nowhere to go. It backs up directly into the pancreatic beta cells, permanently jamming the ATP synthase rotors and forcing an eventual, catastrophic Landauer liquidation, yielding rapid regain of high-viscosity fat mass, thyroid C-cell risks, and structural insulin burnout.
The lesson of the Bar-tailed Godwit is absolute: you cannot safely alter metabolic time flow or handle massive energy conversions without an active, material dielectric shield to ground the spin noise. Humans using RETA cannot grow a pecten oculi, but through the direct application of decentralized physics, we can manually build its functional equivalent.
If a modern human is navigating a changing environment or using targeted peptides, they must deploy the macro-scale boundary conditions that centralized medicine ignores:Rebuilding the Melanin Grid: Throwing away the sunglasses and chemical sunscreens to allow natural, latitude-based full-spectrum light to initiate dermal pooling, restoring triplet-state oxygen and charging the water table back to (k = 160).
Mechanical Common-Mode Rejection: Wearing a Spurling chiral neck loop precisely over the vagal and carotid choke points to filter out transverse field noise, creating an active longitudinal scalar column that assists the body in clearing deuterium grease from the brain-gut axis.
The High-Dielectric Buffer: Utilizing Sunlight and my cold thermogenesis protocol while being grounded to paramagnetic basalt soil dressings to manually clear the bicarbonate exhaust pipe, preventing the anomalous volume isotope expansion that forces cells to swell like CME-stressed ice cubes. The phsyics scales from ice cubes to you.
8. You thought I was joking about ice cubes and obesity being linked to D+. Read some more.
https://x.com/DrJackKruse/status/2062702566664708194
9. I am not playing around with the TARD army any longer. They are harming millions with their bad science and the paid influencer class.
https://x.com/DrJackKruse/status/2062781354828234764
10. If you do not think those who power the science care little for humanlife, you clearly are not paying attention.
Here is how things should be framed about Rockefeller Medicine but are not because the bankers control the media.
Here is how things should be framed about Rockefeller Medicine but are not because the bankers control the media.
https://x.com/DrJackKruse/status/1990565463437312181
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