Mark Kelley ND, LAc

The popular joint supplement glucosamine has been linked to a 25% faster progression from mild cognitive impairment to Alzheimer’s disease. A major new study published in Nature Metabolism has revealed a concerning association between glucosamine, a widely used over-the-counter supplement for joint pain, and accelerated cognitive decline. Researchers at the University of Florida analyzed 12 years of electronic health records and found that patients with mild cognitive impairment (MCI) who regularly took glucosamine were 25% more likely to progress to full Alzheimer’s disease compared to non-users. The risks extended further: among individuals already diagnosed with dementia, glucosamine use was associated with a 25% higher mortality risk. Scientists believe the supplement may worsen the condition because glucosamine readily crosses the blood-brain barrier and fuels an overactive “sugar-tagging” (hyperglycosylation) pathway in vulnerable brains, aggravating metabolic dysfunction. Importantly, this risk appears to be specific to people whose brains are already undergoing neurodegeneration. In healthy individuals, some earlier research has actually suggested potential protective effects. However, with tens of millions of people — many of them older adults — taking glucosamine for joint health, these findings highlight the need for caution and further clinical trials. [Hawkinson, T. R., Gentry, M. S., & Sun, R. et al. (2026). Hyperglycosylation is a metabolic driver of Alzheimer’s disease. Nature Metabolism. DOI: 10.1038/s42255-026-01538-4]

Todd had terminal ALS and just ordered a wheelchair—then DMSO gave him his life back His brain fog vanished. Breathing crises stopped in 3 days. He dragged 340-lb beams across a road. His reflexes healed. His recovery shocked his doctors—but ALS is far from the only thing DMSO helps. James Miller MD found roughly 80% of neurological issues people see neurologists for simply go away once he gives them DMSO. Approximately 2500 studies support its use for conditions ranging from Alzheimer’s and Parkinson’s to strokes, MS, paralysis, chronic pain, spinal injuries, depression, epilepsy, and Down syndrome. Here, I will show how DMSO can cure many "incurable" neurological disorders.🧵

This is a clip that is so on point it may be very uncomfortable for some to watch. However, the Chinese man featured in the clip is saying out loud what I have written about at length and many academics have articulated. You’ll have to excuse the captions which struggles with his Chinese accent, but that doesn’t detract from the message. 🎥 TikTok - https://t.co/FvZxHZpe4Z

Dr David Morris exposes Cortisone shots are used a revenue generator by Big Pharma He reveals they are a scam and “designed to fail” “Here's something orthopedists know, but they're not gonna tell you. And yes, I'm being a little bit cynical here, but cortisone shots are designed to fail. Not by accident, they're designed that way. When you get a cortisone injection, it works for a few weeks or a few months. The pain goes away. You think it's healing, but cortisone doesn't heal anything. It's a powerful anti-inflammatory. That temporarily suppresses the pain signals. Meanwhile, it's actively degrading, it's actively breaking down the tissue. Look this up, don't take my word for it. Cartilage, tendons, ligaments actively being degraded. So when the cortisone wears off, your joint is actually worse than before. The pain can come back stronger. What happens then? Well, then your doctor gives you another shot. After 3 or 4 shots, the cartilage is so degraded that conservative treatment isn't working anymore. Now you're a surgical candidate. This is exactly what the business model requires. Your orthopedist isn't trying to heal your joint with cortisone. He's buying time until you're bad enough to operate on, because that's when he gets paid the most. Again, I'm being cynical, I know that, but it's so frustrating to me” Here’s what you should do “Compare that to regenerative medicine. When we inject Wharton's jelly or PRP, platelet-rich plasma, we're triggering a healing response. Growth factors, cytokines, signaling molecules that tell your body to repair tissue and build new collagen. It takes longer, it costs more upfront, but you're actually healing. We're not just masking symptoms while the problem accelerates towards surgery” “So if your orthopedist recommends another cortisone shot, ask him, what's the plan after this stops working? Because if the answer is surgery, he's not treating you, he's preparing you” He’s 100% right Cortisone shots repeated use is linked to: - Tissue degradation - Cartilage thinning and accelerated osteoarthritis progression - Tendon weakening or rupture - Bone death, joint infection, skin atrophy, and faster joint deterioration So what are the real treatment options? I found those too PRP (Platelet-Rich Plasma): Uses your own blood’s concentrated growth factors to stimulate repair, collagen production, and reduce inflammation. Studies often show better long-term pain relief and function (6–12+ months) compared to cortisone, fewer risks of tissue breakdown Wharton’s Jelly (Umbilical Cord MSCs): Contains mesenchymal stem cells, growth factors, and anti-inflammatory components from donated umbilical cords. Early evidence suggests it can help with pain, mobility, and tissue repair in joints Our healthcare system isn’t about fixing you, it’s about long term customers and repeated treatments

🚨 EVERY VACCINE BATCH HAD A DIFFERENT FORMULA. THE LOT NUMBERS JUST PROVED IT. Not a theory. Not an interpretation. A dataset. 12,000 lot numbers. Cross-referenced with VAERS adverse event reports. The correlation is absolute. A team of researchers — 4 statisticians, 2 pharmacologists, 1 former FDA regulator — published their findings on a decentralized server Wednesday. The paper is 147 pages. Peer review was impossible because no journal would touch it. So they released it directly to the public. The finding: specific lot numbers produced 4,000% more adverse events than others. Not random variation. Not manufacturing inconsistency. A deliberate, systematic pattern. ⟁ Lot numbers ending in 20A through 20F: near-zero adverse events. Saline. Placebo. Water with a label. Lot numbers ending in 21K through 21X: moderate adverse events. Fatigue. Myocarditis. Blood clots. Hospitalization rates 300% above baseline. Lot numbers ending in 22R through 22Z: catastrophic. Stroke. Cardiac arrest. Neurological damage. Death rates 8,100% above the statistical norm for any pharmaceutical product in history. Three tiers. Three formulas. Distributed in a pattern that ensured no single hospital, no single city, no single demographic received enough catastrophic doses to trigger an obvious statistical signal. They spread the damage thin enough to call it "rare side effects." But it wasn't rare. It was targeted. ⟁ The distribution pattern wasn't random. The catastrophic lots were sent disproportionately to specific zip codes. Zip codes with high concentrations of military veterans. First responders. Independent business owners. Communities with historically low compliance to federal mandates. The people most likely to resist were given the most dangerous doses. The moderate lots went to urban centers with high media consumption — populations that would report mild symptoms, be told it was "normal," and return for boosters without question. The placebo lots went to politicians, media figures, and pharmaceutical executives. The people who promoted it on camera. The people who told you it was "safe and effective" while receiving saline. They took the same shot on television. They did not take the same formula. ⟁ The 12,000 lot numbers are now mapped. Every batch. Every destination. Every outcome. The data is on the blockchain. It cannot be retracted. It cannot be memory-holed. It cannot be fact-checked into oblivion. The former FDA regulator on the team submitted the dataset to the military tribunal with a single statement: "This was not negligence. This was a weapons deployment protocol disguised as public health." The tribunal accepted it into evidence Thursday morning. Case number: GT-2026-0441. Every lot number is a fingerprint. Every adverse event is a witness. Every death certificate is an indictment. CODE: LOT-NUMBERS / 3-TIERS / ZIP-TARGETED / GT-2026-0441 They didn't give everyone the same shot. They gave everyone the shot they were assigned. Now the assignment list is evidence. ♟ Someone you know got a different formula than they were told. Share this for them. Mr Pool

Dr. A is one of my members. Love his energy to treat patients with truth. I am going to upgrade this tweet. WHY MIGHT CENTRALIZED MDs RETAIN THE BELIEF STATINS HELP? I believe they retain the belief because almost all of their patients are heavily deuterated by the Rockefeller paradigm that control Big Ag and water since the 1940s, so when centralized MDs are taught by the Rockefeller paradigm to give them a drug that is a mitochondrial toxin, realize why they are doing it. Giving a mitochondrial toxin would slow the RPM rate of the ATPase along the IMM from NADD+ ---> O2, effectively preventing the shreding of their cardiac muscle fibers. How is that for a decentralized reality check. This is the ultimate Decentralized Medicine's "Biophysical Reality Check." Decentralized medicine looks at patients differently because they put BIOPHYSICS > PHARMACOLOGY. This idea identifies why a mitochondrial poison can appear "cardioprotective" in a dying magentic system: Statins act as a "Governor" on a runaway, "knocking" engine. If a patient is heavily deuterated, their mitochondrial motors are "stuttering" and "arc-welding" their own cristae. In that specific, high-entropy state, slowing the motor down with a toxin prevents it from physically shredding the cell. This explains to you, why the Rockerfeller Dynasty knows precisely what they have been doing to America food supply. They are behind the deuterium bomb food problem so they sell a pill that they know everyone needs so they do not die of dilated cardiomyopathy so they can sell them drugs for a longer period of time. 1. The "ATPase Shrapnel" Effect In a system with a dielectric constant of 78 (bulk water) instead of 160 (structured DDW), the water is too viscous to handle the 9,000 RPM of the ATPase. The Stall: As I discussed, a D+ "speed bump" hits every 4.3 seconds at 155 ppm. The Damage: At 40 million V/m, these collisions aren't just "slow-downs"; they are kinetic explosions. The ATPase "shudders," creating mechanical shear stress that tears at the cardiac muscle fibers and the IMM. The Statin "Fix": By inhibiting the mevalonate pathway and CoQ10, statins starve the motor of torque. This eliminated the problem the Mayans faced in theri magnetic decline. Rockefeller medicine needs their victims not to feel the flutter in the chest, so they lower the RPMs of the ATPase to hide the effect of their real agenda. This is why they have their own food supply. To an MD, the reduction in "cardiac enzymes" (muscle damage markers) looks like "protection," but it’s actually just slowing the rate of destruction by making the engine too weak to "knock" its way through the sludge. 2. The Uncontrolled Variable: Isotopic Silt I just gave you the "Smoking Gun" of clinical research: Deuterium is the Great Uncontrolled Variable. Every statin trial is conducted on a population living in "Magnetic Darkness" (indoors, high nnEMF, high declination) and drinking 155 ppm water. In this "78-dielectric" cohort, a mitochondrial inhibitor will show a benefit because it prevents the "Isotopic Flashover." The Centralized Allopathic Blindness: They see "lowered cholesterol" and "reduced events" and assume the drug is a "miracle." They don't realize they are just dimming the lights in a house that’s about to have an electrical fire. 3. The "Stall" as a Proxy for "Stability" Centralized medicine confuses "Inertia" with "Health." A healthy heart should have high Vortex Torque and a Light Lattice (160). A "Statin-protected" heart has Low Torque and a Heavy Lattice (78). Because the "heavy" heart is too weak to trigger a massive, sudden "Singlet Flashover" (MI), the clueless allopath calls it "stable." It is the stability of a cemetery. 4. The "Heme-Melanin" Divorce Statins interfere with the very Heme renovation I’ve been discussing on the blogs in the Decentralized Medicine series. By lowering the mitochondrial capacity, they ensure the Isotopic Filter (CCO) never reaches its "Cambrian" efficiency. The patient remains trapped in the Warburg/Atavistic state. They don't die of a heart attack today, but they "brown" into Amyloidosis, Ataxia, or SAA-era Dementia tomorrow. They know exactly what they doing and they paying PhDs to produce science that will never show the answer. MDs do not know shit about the dielectric table. 5. The Synthesis: The "Grounded" Alternative If those same patients were on 92.5 ppm DDW and 3% NaCl, their dielectric constant would return to 160. The water would be "frictionless." The 9,000 RPM motor would spin without "shredding" the fibers. The "Statin" would then be revealed for what it truly is: a Quantum Brake that prevents the heart from reaching its 160THz potential. My Decentralized Conclusion: Allopathic "success" with statins is the Proof of Universal Human Deuteration. They are "solving" the problem of Isotopic Friction by killing the Mitochondrial Vortex. The Reality Check: Centralized cardiologist's are not "preventing" muscle damage; they are crippling the engine so it can't feel the "Speed Bumps," so you remain comfortbly numb to the paradigm agenda and they keep you as a long term customer. Just think like a Banker, because that who runs BigHarma retards.