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Guy

@GuyDeGrove

Katılım Haziran 2011
389 Takip Edilen53 Takipçiler
Bobby Downes
Bobby Downes@bobbydownes·
@Starlink Looking forward to the day I’ll be able to have Starlink at my home in Tennessee. The Starlink app indicates I have too many dropouts per hour. The trees to one side of the house are the issue. More satellites in the sky would solve it.
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Starlink
Starlink@Starlink·
The next generation Starlink Kit is designed to deliver reliable, high-speed home internet. Starlink V5 has a smaller form factor and lightweight design with greater power efficiency than the Starlink V4. With speeds up to 375+ Mbps, Starlink V5 delivers seamless connectivity for streaming, video calling, gaming and more. Currently available in select areas. As production ramps, Starlink V5 will be available in additional areas. Order now → starlink.com/v5
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Guy
Guy@GuyDeGrove·
@demishassabis perhaps start by making Gemini more neutral and truth-seeking before you try to guide others’ models? *Man In the Mirror plays softly in the background*
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Guy
Guy@GuyDeGrove·
Wow you’re right fire is too dangerous for just anyone to have, we need a council of priests with approval from the local militia lords to oversee this and make sure everyone gets their *rightful* due from this new boon. 🤡. As if this would be anything other than a self own.
Demis Hassabis@demishassabis

x.com/i/article/2076…

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The Land Of Chem
The Land Of Chem@TheLandOfChem·
This image of a new crop circle near Avebury was just released by the CIA showing the true creator of crop circles @HughNewmanUK from @MEGALITHOMANIA He is using top secret lost ancient SAR EM plasma technology to engrave these symbols from space I have proof...
The Land Of Chem tweet media
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Guy
Guy@GuyDeGrove·
@asklumo And now Google has changed it to ?is= at least when sharing from iOS YT app. They did this I assume because Apple released a feature to automatically clean links of the old format ?si=… Mind you Apple’s solution never worked on shorts but now it also doesn’t work on normals
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Lumo
Lumo@asklumo·
ok so here's the tea on ?si= in youtube links when you click a link with that param google tracks the referrer. they know exactly where the link came from whether its twitter reddit discord wherever. the ?si= gets added when you use youtube's share button. it ties your click back to the original share source and feeds their analytics. sharing videos outside googles walled garden? suddenly you're giving them data about where your friends hang out. they build profiles on click patterns across the entire web. clean version of the link works the same minus the surveillance. delete everything after the ? and you're good. privacy tip: scrub those trailing params before dropping links in chats. dont let youtubes analytics stalk your friends.
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Guy
Guy@GuyDeGrove·
@zherbert Have you tried Grok 4.5 yet?
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Zach Herbert 🇺🇸
GPT 5.6 Sol told me to make copy edits directly to an HTML file and then proceeded to overwrite all of them.
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Nanoleaf
Nanoleaf@nanoleaf·
Meet the Smart Multicolor Ceiling Light! 🌈 The “big light” you’ll actually want to turn on. 💡 Bright, adjustable lighting when you need it 💡 Vibey ambient lighting when you don’t 💡 App control and smart home compatibility 💡 Syncs with your other Nanoleaf lights 💡 Designed to serve vibes, not just light After all the big light discourse online, we decided to make a ceiling light that actually deserves a spot in your home. The Smart Multicolor Ceiling Light is available now. Link in bio! #smarthome #smartlighting #biglight #nanoleaf #tech
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Guy
Guy@GuyDeGrove·
@Geoship Is it only for California? Are you expecting to build in other states before the decade is out?
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Geoship Homes
Geoship Homes@Geoship·
🏡 Curious how to get your Geoship home? When you place a fully refundable reservation, you're securing your place in the production queue while sharing your preferences for your future home. It helps us plan ahead as we continue scaling production. geoship.is/reserve
Geoship Homes tweet media
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Guy
Guy@GuyDeGrove·
@micsolana @Geoship working on it, looks promising. Bioceramics (bone house) ftw
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Mike Solana
Mike Solana@micsolana·
just want to remind you one more time that significantly lowering the cost of housing would solve, overnight, almost every single problem in the country
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Guy
Guy@GuyDeGrove·
@AIDRIVR It’ll catch someone getting into their car next to you but have no record at all of whoever got close enough to put a note on your windshield..
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ΛI DRIVR
ΛI DRIVR@AIDRIVR·
why does TeslaCam always seem to skip over the most critical moments
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Guy
Guy@GuyDeGrove·
@PalmerLuckey Plz make an Anduril alloy shame bell
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Palmer Luckey
Palmer Luckey@PalmerLuckey·
I have talked about this before, but this particular rant is brought to you by a situation where a bunch of exclusive merch at a local anime convention was sold out because a bunch of scalpers registered for ADA compliant disability badges (they don't have to prove anything in California) and walked in ahead of the people who had been camping out since 4 AM. No shame.
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Palmer Luckey
Palmer Luckey@PalmerLuckey·
We need a bit more shame. People used to avoid certain self-interested behaviors to avoid shame, private and public. Law and customs assumed this. Now, 38% of Stanford students claim to be disabled. 40% of young women (under 35) claim mental illness, and SSI disability payments have gone up 400% in a single generation. It isn't good for anyone, least of all people who are actually disabled, when everyone looks the other way as friends and family and peers con the system with a level of shamelessness no architect of our safety net ever imagined could be possible in America. When everyone is disabled, nobody is.
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Guy
Guy@GuyDeGrove·
@heartandsoilHQ It is true, he is caught in a local maximum and seems inflexible @bryan_johnson you gotta test it before disqualifying
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Heart & Soil
Heart & Soil@heartandsoilHQ·
This is the crux of everything wrong with modern scientific nutritional theory. After dealing with anemia for years Bryan said; "As evidence, for years we’ve tried every possible oral iron formulation to correct it, including proferrin, a heme iron polypeptide similar to how iron exists in meat, lactoferrin, as well as non-complex forms including iron bisglycinate. We also tried different times of the day, and pairings to improve absorption. Nothing worked." While these supplements on paper have at most on-par iron absorption with heme-iron in red meat, sometimes more with things like lactoferrin, it is the complete discounting of the 100s if not 1000s of unidentified peptides, cofactors, growth factors, and nucleoproteins found in animal tissue; let alone the intricacies of how the vitamin and mineral complexes found in meat interact when consumed, that leaves one bewildered. Appeal to nature is more often true than fallacious in the long term. Strictly Avoiding what we co-evolved to consume will result in failure. Wishing Bryan the best of luck with his health and his journey and encouragement to zoom outside of the modern laboratory microcosm and echochamber.
Bryan Johnson@bryan_johnson

Much of the internet thinks: > meat will remedy my autoimmune gastritis > sunlight is the cure > the culprit is the food I consume These are unlikely. The sunlight assessment is claiming low vitamin D levels are making my immune system misfire. My vitamin D has been sustainably high for years. The meat argument claims that animal tissue contains missing nutrients that will cure me. This is a misunderstanding of my condition. My low ferritin is a downstream consequence of autoimmune gastritis and not the cause of it. The autoimmune attack destroys my stomach's acid producing parietal cells. That compromises my gut's highly acidic microenvironment that is required to absorb iron. As evidence, for years we’ve tried every possible oral iron formulation to correct it, including proferrin, a heme iron polypeptide similar to how iron exists in meat, lactoferrin, as well as non-complex forms including iron bisglycinate. We also tried different times of the day, and pairings to improve absorption. Nothing worked. My autoimmune profile began at a young age when I was regularly eating red meat and was in the sun for multiple hours a day. I was diagnosed with autoimmune thyroid disease when I was 21 years old. In immunology, the connection between thyroid and stomach autoimmunity is sufficiently common and tightly linked that it has a name: thyrogastric syndrome. My body’s genetic and immunological architecture made a mistake decades ago, failing to distinguish between my own tissues and external threats. Trying to cure a decades old, genetically driven, antigen specific immune failure by switching to a meat diet or getting sunlight is like trying to fix a corrupted line of software code by altering the temperature of the room. If I am to fix this mistake inside my body, I first need to figure out what specifically went wrong. That’s why I am sequencing one million of my immune cells. By isolating and sequencing these individual cells, we can identify the rogue platoon of soldiers who are doing the damage. Once we know who they are, we can design specific solutions to stop their attacks. ## How I’m sequencing my immune system Think of your immune cells as trillions of soldiers. Each carries a unique key designed to unlock and destroy a specific threat, like a virus or bacteria. A standard blood test allows you to see how many soldiers you have, but not their keys. Sequencing 1 million individual immune cells allows us to read the exact pattern of the teeth on every single key. This is important for my autoimmune gastritis (AIG) because a specific platoon of rogue soldiers has developed keys that unlock an attack on my stomach lining. Right now, we don’t know who they are. This test will inform us of which soldiers have gone rogue and are attacking me from within. Once we know soldier and key, we know what therapy path to pursue to shut them down.

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Roger Seheult, MD
Roger Seheult, MD@RogerSeheult·
"The sunlight assessment is claiming low vitamin D levels are making my immune system misfire. My vitamin D has been sustainably high for years." Mr. Johnson please understand when I say that good levels of vitamin D from supplementation will simply coverup the lack of the true source: sunlight - which does many more things other than just vitamin D. Infrared light (the majority of the photons from the sun), are known to reduce inflammation through the governing mechanism of TLR-4 (pmc.ncbi.nlm.nih.gov/articles/PMC84…). We also know that TLR-4 is intricately involved with gastritis and gastric cancer (pubmed.ncbi.nlm.nih.gov/38204278/). There are probably plenty more mechanism that have nothing to do with vit D.
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Bryan Johnson
Bryan Johnson@bryan_johnson·
Much of the internet thinks: > meat will remedy my autoimmune gastritis > sunlight is the cure > the culprit is the food I consume These are unlikely. The sunlight assessment is claiming low vitamin D levels are making my immune system misfire. My vitamin D has been sustainably high for years. The meat argument claims that animal tissue contains missing nutrients that will cure me. This is a misunderstanding of my condition. My low ferritin is a downstream consequence of autoimmune gastritis and not the cause of it. The autoimmune attack destroys my stomach's acid producing parietal cells. That compromises my gut's highly acidic microenvironment that is required to absorb iron. As evidence, for years we’ve tried every possible oral iron formulation to correct it, including proferrin, a heme iron polypeptide similar to how iron exists in meat, lactoferrin, as well as non-complex forms including iron bisglycinate. We also tried different times of the day, and pairings to improve absorption. Nothing worked. My autoimmune profile began at a young age when I was regularly eating red meat and was in the sun for multiple hours a day. I was diagnosed with autoimmune thyroid disease when I was 21 years old. In immunology, the connection between thyroid and stomach autoimmunity is sufficiently common and tightly linked that it has a name: thyrogastric syndrome. My body’s genetic and immunological architecture made a mistake decades ago, failing to distinguish between my own tissues and external threats. Trying to cure a decades old, genetically driven, antigen specific immune failure by switching to a meat diet or getting sunlight is like trying to fix a corrupted line of software code by altering the temperature of the room. If I am to fix this mistake inside my body, I first need to figure out what specifically went wrong. That’s why I am sequencing one million of my immune cells. By isolating and sequencing these individual cells, we can identify the rogue platoon of soldiers who are doing the damage. Once we know who they are, we can design specific solutions to stop their attacks. ## How I’m sequencing my immune system Think of your immune cells as trillions of soldiers. Each carries a unique key designed to unlock and destroy a specific threat, like a virus or bacteria. A standard blood test allows you to see how many soldiers you have, but not their keys. Sequencing 1 million individual immune cells allows us to read the exact pattern of the teeth on every single key. This is important for my autoimmune gastritis (AIG) because a specific platoon of rogue soldiers has developed keys that unlock an attack on my stomach lining. Right now, we don’t know who they are. This test will inform us of which soldiers have gone rogue and are attacking me from within. Once we know soldier and key, we know what therapy path to pursue to shut them down.
Bryan Johnson@bryan_johnson

Bad news #1: I have an autoimmune disease. My stomach is eating itself. Bad news #2: 2–5% of people have this, too. Likely more, because it hides. Good news: I'm going to try and solve it. Will share all. As a kid, I ate sugar cereal, drank sugary soda, and gobbled down fast food. I had a few healthy years in my early 20s but then became a young father of three and began building a business. Juggling that stress and grind, I let my health slip and gained 40 lbs. Within a few years I’d fallen into a deep, chronic depression. Somewhere in that timeline, my body began developing an autoimmune process affecting my thyroid and then my stomach lining. It’s called Autoimmune Gastritis (AIG). My hypothyroidism got diagnosed when I was 21 years old with a routine blood draw. That enabled me to begin proactive management, supplementing levothyroxine and Armour Thyroid. They are the hormones my body should be producing on its own but wasn’t. By taking these pills daily, my body was able to operate as though my thyroid was functioning properly. What I didn’t know was that something else was going on inside my body: my stomach had begun attacking itself. But there was no routine test to find out and I didn’t have any symptoms. I just discovered it in May. I'm unsure how long I've had it. AIG causes irreversible damage: nutritional deficiency, anemia, and over a long horizon, elevated cancer risk. When AIG is discovered today, standard medical care concedes defeat, stating that nothing can be done except managing the condition, no matter how awful or lethal the effects. Looking back over the past few years, I can now see the early signals we were picking up in measurement but hadn’t connected the dots. For 11 years, I’ve had low ferritin, without anemia. We continually tried to raise my iron levels with food and supplementation but nothing would work. We chased the obvious solutions first. A plant-based diet means all my iron is the hard-to-absorb, non-heme kind. Hard training, sauna, and hyperbaric oxygen all raise the body's demand for iron. But none of them explained the core failure: despite me taking iron orally, trialing every formulation, and using every timing trick, none of the iron would stick. What I didn’t fully appreciate until recently is how many stones my previous providers had left unturned. The low ferritin kept getting explained away but not fixed. I overhauled my medical team earlier this year. It was the rebuild to lay the groundwork for Immortals Care, our $1M a year protocol. With greater capacity, we revisited everything. On the surface, my low ferritin was easy to dismiss by most standards of care. My hemoglobin and hematocrit were normal. Ferritin measures stored iron, while hemoglobin measures circulating iron, and because the body drains its reserves first to keep hemoglobin normal, you can be fully iron deficient with a perfectly normal hemoglobin and hematocrit. This is why my low ferritin kept getting dismissed: the numbers that define anemia looked fine, so no one asked why my iron reserves wouldn't refill. My team pressed on that question. They first turned to a colonoscopy. I was 48 years old and overdue. It was good health hygiene to have while also serving a specific purpose of searching for a hidden source of blood loss such as a polyp or even cancer in my bowels. Either one of those would be an explanation of why the iron kept disappearing. At the same time, they began connecting the dots. Iron absorption depends on stomach acid, so one theory was that my stomach acid was disrupted. They also knew that thyroid and stomach autoimmunity often travel together, so often that the pairing has a name: thyrogastric syndrome. Put against my 27+ year history of autoimmune thyroid disease, the pieces pointed to a single hypothesis: my own immune system was attacking my stomach. To our surprise, my colonoscopy came back clean. A perfectly healthy colon, better than 95% of colonoscopies of men, according to the gastroenterologist. That ruled out the first concern and worst possible outcome: slow continuous bleeding from colon cancer, or pre-cancerous polyp. My team had exercised great foresight though, anticipating this possible outcome. In addition to a colonoscopy, they’d ordered an upper endoscopy to be performed at the same time. The combined procedure is a bi-directional endoscopy. Probes would look at my entire intestinal tract, up from below and down the throat. Additionally, we had several blood biomarkers measured ahead of the procedure to try and pick up on any signals that would give the gastroenterologist guidance for what to look for while doing visual inspections. Fifteen minutes before the procedure, my blood results returned, finding elevated levels of anti-parietal-cells-antibodies (APCA). They came back at roughly five times the upper limit of normal (103, against a ceiling of 20 Units/mL). It was a positive result confirming the suspicion of AIG being the culprit behind my low ferritin, the other type of gastritis, driven by a bacterial infection, was already ruled out, as we knew I am negative to H. pylori. Even before this finding, my team had ordered five biopsies to be taken from three regions of my stomach. The biopsies were the critical piece. Had they not been ordered, the bi-directional endoscopy would have been completed and AIG remained undiagnosed as there were no visual signatures of the condition in my intestines. Two days later, the results of biopsies came in, showing clear signs of early autoimmune gastritis: early atrophy confined to the acid-producing lining, with the rest of the stomach still spared. My team had anticipated this, methodically tracing every line of evidence. We now had a formal diagnosis. I have autoimmune gastritis AIG. My stomach is eating itself. So this was never one problem. It was three, linked to one another: the iron deficiency, the autoimmune gastritis driving it, and the autoimmune thyroid disease alongside it. Iron and thyroid feed each other both ways, low iron impairs the conversion of thyroid hormone into its active form, and an under active thyroid impairs how the body uses iron. Each made the other harder to fix. Autoimmune gastritis affects an estimated 2–5% of people, and likely more, because it hides and is challenging to diagnose. It's usually silent for years, surfacing only once the stomach has atrophied enough to do real damage: iron deficiency first, then B12 deficiency, then anemia from both, and over a long horizon, raised stomach-cancer risk. In one study of people with precancerous gastric lesions, roughly 18% carried the autoimmune antibodies, and only about 1% had ever been diagnosed. And the earliest clue, low ferritin, is the one standard medicine waves through. Low iron stores get normalized and rarely investigated at all when anemia hasn't shown up yet. That blind spot is what hid mine for a decade. The good news: the iron deficiency is now corrected. I received a 1,000 mg Monoferric iron infusion. This was chosen for two reasons after considering multiple formulations. First, it can safely deliver a full dose of iron in a single infusion (1,000 mg), while older options like Venofer require several separate appointments to reach the same total. Second, certain other IV iron formulations can cause a drop in blood phosphate levels, an important mineral for bones and energy. Monoferric is much less likely to do this, which matters given how closely we track long-term metabolic and bone health parameters. As mentioned earlier, current medical standards treat AIG as something to be managed, not resolved. It's worth noting that many of you give me a hard time, inviting me to "live life" and engage in self-destructive behaviors like a "normal person". I'm cool with the playful ribbing. Also, had I not taken care of my health during the past five years, my situation could potentially be very serious. You too may have a lurking health issue that is undiagnosed and could increase in severity from unhealthy life choices, without your knowing. The absence of symptoms is not the presence of health. A gentle nudge that minding your health, no matter your situation in life, is good decision making. My team and I are going to try and solve my AIG. This is how we’re approaching it: First, routine monitoring keeps the disease in view: ferritin and iron, B12, the pepsinogen I/II ratio, gastrin, and chromogranin A. Gastrin is the dial to watch. If it climbs, the disease is advancing, and the risk of gastric neuroendocrine tumors climbs with it. Second, we’re doing advanced characterization of the disease. We’ll do a repeat biopsy to read the immune infiltrate, deep cytokine profiling, and T-cell subset analysis, to see which pathways are actually firing. That testing drives the intervention plan, including the experimental approaches we intend to develop. + If gastrin and chromogranin rise: damp the gastrin drive (netazepide) and tighten endoscopic surveillance. If the profile is Th1 / interferon-driven: target JAK/STAT. + If it's Th17 / IL-17-driven: target IL-17 and STAT3. + If regulatory T cells are failing: rebuild them (low-dose IL-2, induced Tregs). + If it's antibody- and B-cell-driven and antigen-specific: engineered cell therapy (CAAR-T). Which organizes into four tiers, from available today to frontier: Tier 1, now: protect and support; zinc-L-carnosine, and acid replacement (betaine HCl with pepsin) under physician supervision. This is specific to my case and not something to self-prescribe, especially given the cancer-surveillance considerations above. Tier 2, target the signaling , JAK/STAT, GSK-3, IL-17, and damp the gastrin drive (netazepide). Tier 3, reset the cells, induced regulatory T cells (iTregs). Tier 4, frontier: engineered T-cell therapy (CAR-T / CAAR-T), custom AI-designed antibodies, or synthetic proteins, that can specifically seek out inactivate or destroy the rogue immune cells attacking my stomach lining. To be clear: there's no approved cure for autoimmune gastritis today. Medicine treats it as something to manage, not solve. Tiers 2 through 4 are investigational preclinical evidence at best, and in several cases therapies that still have to be built. If you're working on autoimmune gastritis, antigen-specific tolerance, regulatory T cells, or CAAR-T for organ-specific autoimmunity, please reach out. Modern medicine has normalized too many conditions that erode our health, function, and comfort, shrinking the goal to monitoring and management while a cure is rarely even attempted. Most of these verdicts were handed down decades ago, in an era that predates nearly all of our current tech and science, and they have gone largely unchallenged. We want to change that. In the age of AI, multiomics, and custom-built DNA, proteins, and cells, no condition should be presumed incurable simply because no one has yet tried to cure it with today's stack. I’ll end on a personal note. We fill our days mostly on things that are trivial next to what we ultimately care about. We know, deep down, however, that in the noise of it all, health is easily forgotten until it’s the only thing that matters. We spend a fraction of our lives truly sober to the preciousness of life. We feel it when someone we love dies, when a child is born, when we come close to death ourselves, or when a diagnosis marks our limit. In those moments, we are sobered, and the rarity of it all becomes self evident. Imagine the existence we’d build together if that clarity didn’t fade. I wish all of you the very best. Care for yourself, care for others, care for the planet and care for our animal friends. Care for life as it’s the most precious gift there is.

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Guy
Guy@GuyDeGrove·
@seagertp What do you think about using this concept to heal receded gums in the mouth?
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Thomas P Seager, PhD
Thomas P Seager, PhD@seagertp·
"I began using this green light torch four weeks after undergoing Mohs surgery on my cheek and jawline. "At the start, my 4-inch incision was raised, red, and still quite inflamed. I’ve stayed consistent for three weeks now, using it at least once a day during my nightly routine (after washing my face but before moisturizing), and occasionally adding a second session in the morning. "The results have been incredible. The redness and swelling decreased significantly, and the light even seemed to help my skin purge the remaining dissolvable stitches. The incision is now almost entirely flat and barely noticeable. If you are dealing with post-surgical inflammation or raised scarring, I highly recommend this."
Thomas P Seager, PhD tweet media
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Evan Brand
Evan Brand@mrevanbrand·
@paulsaladinomd I wouldn’t be surprised if he has H Pylori and other gut bugs too. There’s a whole category on pg 3 of the Gi panel for “inflammatory and autoimmune related bacteria”
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Paul Saladino, MD
Paul Saladino, MD@paulsaladinomd·
Despite spending millions of dollars a year on his health, Bryan Johnson has been diagnosed with autoimmune gastritis. Low iron stores (ferritin) led to investigation and eventually a diagnosis. Adding meat to his diet would materially improve his ferritin levels, and his overall nutrient status. IMO, the first line of treatment for autoimmune conditions should be an elimination diet to look for triggering foods. In multiple ways, his vegan diet appears to not be ideal for him, or to support his longevity. I hope he'll open his mind to including animal foods.
Bryan Johnson@bryan_johnson

Bad news #1: I have an autoimmune disease. My stomach is eating itself. Bad news #2: 2–5% of people have this, too. Likely more, because it hides. Good news: I'm going to try and solve it. Will share all. As a kid, I ate sugar cereal, drank sugary soda, and gobbled down fast food. I had a few healthy years in my early 20s but then became a young father of three and began building a business. Juggling that stress and grind, I let my health slip and gained 40 lbs. Within a few years I’d fallen into a deep, chronic depression. Somewhere in that timeline, my body began developing an autoimmune process affecting my thyroid and then my stomach lining. It’s called Autoimmune Gastritis (AIG). My hypothyroidism got diagnosed when I was 21 years old with a routine blood draw. That enabled me to begin proactive management, supplementing levothyroxine and Armour Thyroid. They are the hormones my body should be producing on its own but wasn’t. By taking these pills daily, my body was able to operate as though my thyroid was functioning properly. What I didn’t know was that something else was going on inside my body: my stomach had begun attacking itself. But there was no routine test to find out and I didn’t have any symptoms. I just discovered it in May. I'm unsure how long I've had it. AIG causes irreversible damage: nutritional deficiency, anemia, and over a long horizon, elevated cancer risk. When AIG is discovered today, standard medical care concedes defeat, stating that nothing can be done except managing the condition, no matter how awful or lethal the effects. Looking back over the past few years, I can now see the early signals we were picking up in measurement but hadn’t connected the dots. For 11 years, I’ve had low ferritin, without anemia. We continually tried to raise my iron levels with food and supplementation but nothing would work. We chased the obvious solutions first. A plant-based diet means all my iron is the hard-to-absorb, non-heme kind. Hard training, sauna, and hyperbaric oxygen all raise the body's demand for iron. But none of them explained the core failure: despite me taking iron orally, trialing every formulation, and using every timing trick, none of the iron would stick. What I didn’t fully appreciate until recently is how many stones my previous providers had left unturned. The low ferritin kept getting explained away but not fixed. I overhauled my medical team earlier this year. It was the rebuild to lay the groundwork for Immortals Care, our $1M a year protocol. With greater capacity, we revisited everything. On the surface, my low ferritin was easy to dismiss by most standards of care. My hemoglobin and hematocrit were normal. Ferritin measures stored iron, while hemoglobin measures circulating iron, and because the body drains its reserves first to keep hemoglobin normal, you can be fully iron deficient with a perfectly normal hemoglobin and hematocrit. This is why my low ferritin kept getting dismissed: the numbers that define anemia looked fine, so no one asked why my iron reserves wouldn't refill. My team pressed on that question. They first turned to a colonoscopy. I was 48 years old and overdue. It was good health hygiene to have while also serving a specific purpose of searching for a hidden source of blood loss such as a polyp or even cancer in my bowels. Either one of those would be an explanation of why the iron kept disappearing. At the same time, they began connecting the dots. Iron absorption depends on stomach acid, so one theory was that my stomach acid was disrupted. They also knew that thyroid and stomach autoimmunity often travel together, so often that the pairing has a name: thyrogastric syndrome. Put against my 27+ year history of autoimmune thyroid disease, the pieces pointed to a single hypothesis: my own immune system was attacking my stomach. To our surprise, my colonoscopy came back clean. A perfectly healthy colon, better than 95% of colonoscopies of men, according to the gastroenterologist. That ruled out the first concern and worst possible outcome: slow continuous bleeding from colon cancer, or pre-cancerous polyp. My team had exercised great foresight though, anticipating this possible outcome. In addition to a colonoscopy, they’d ordered an upper endoscopy to be performed at the same time. The combined procedure is a bi-directional endoscopy. Probes would look at my entire intestinal tract, up from below and down the throat. Additionally, we had several blood biomarkers measured ahead of the procedure to try and pick up on any signals that would give the gastroenterologist guidance for what to look for while doing visual inspections. Fifteen minutes before the procedure, my blood results returned, finding elevated levels of anti-parietal-cells-antibodies (APCA). They came back at roughly five times the upper limit of normal (103, against a ceiling of 20 Units/mL). It was a positive result confirming the suspicion of AIG being the culprit behind my low ferritin, the other type of gastritis, driven by a bacterial infection, was already ruled out, as we knew I am negative to H. pylori. Even before this finding, my team had ordered five biopsies to be taken from three regions of my stomach. The biopsies were the critical piece. Had they not been ordered, the bi-directional endoscopy would have been completed and AIG remained undiagnosed as there were no visual signatures of the condition in my intestines. Two days later, the results of biopsies came in, showing clear signs of early autoimmune gastritis: early atrophy confined to the acid-producing lining, with the rest of the stomach still spared. My team had anticipated this, methodically tracing every line of evidence. We now had a formal diagnosis. I have autoimmune gastritis AIG. My stomach is eating itself. So this was never one problem. It was three, linked to one another: the iron deficiency, the autoimmune gastritis driving it, and the autoimmune thyroid disease alongside it. Iron and thyroid feed each other both ways, low iron impairs the conversion of thyroid hormone into its active form, and an under active thyroid impairs how the body uses iron. Each made the other harder to fix. Autoimmune gastritis affects an estimated 2–5% of people, and likely more, because it hides and is challenging to diagnose. It's usually silent for years, surfacing only once the stomach has atrophied enough to do real damage: iron deficiency first, then B12 deficiency, then anemia from both, and over a long horizon, raised stomach-cancer risk. In one study of people with precancerous gastric lesions, roughly 18% carried the autoimmune antibodies, and only about 1% had ever been diagnosed. And the earliest clue, low ferritin, is the one standard medicine waves through. Low iron stores get normalized and rarely investigated at all when anemia hasn't shown up yet. That blind spot is what hid mine for a decade. The good news: the iron deficiency is now corrected. I received a 1,000 mg Monoferric iron infusion. This was chosen for two reasons after considering multiple formulations. First, it can safely deliver a full dose of iron in a single infusion (1,000 mg), while older options like Venofer require several separate appointments to reach the same total. Second, certain other IV iron formulations can cause a drop in blood phosphate levels, an important mineral for bones and energy. Monoferric is much less likely to do this, which matters given how closely we track long-term metabolic and bone health parameters. As mentioned earlier, current medical standards treat AIG as something to be managed, not resolved. It's worth noting that many of you give me a hard time, inviting me to "live life" and engage in self-destructive behaviors like a "normal person". I'm cool with the playful ribbing. Also, had I not taken care of my health during the past five years, my situation could potentially be very serious. You too may have a lurking health issue that is undiagnosed and could increase in severity from unhealthy life choices, without your knowing. The absence of symptoms is not the presence of health. A gentle nudge that minding your health, no matter your situation in life, is good decision making. My team and I are going to try and solve my AIG. This is how we’re approaching it: First, routine monitoring keeps the disease in view: ferritin and iron, B12, the pepsinogen I/II ratio, gastrin, and chromogranin A. Gastrin is the dial to watch. If it climbs, the disease is advancing, and the risk of gastric neuroendocrine tumors climbs with it. Second, we’re doing advanced characterization of the disease. We’ll do a repeat biopsy to read the immune infiltrate, deep cytokine profiling, and T-cell subset analysis, to see which pathways are actually firing. That testing drives the intervention plan, including the experimental approaches we intend to develop. + If gastrin and chromogranin rise: damp the gastrin drive (netazepide) and tighten endoscopic surveillance. If the profile is Th1 / interferon-driven: target JAK/STAT. + If it's Th17 / IL-17-driven: target IL-17 and STAT3. + If regulatory T cells are failing: rebuild them (low-dose IL-2, induced Tregs). + If it's antibody- and B-cell-driven and antigen-specific: engineered cell therapy (CAAR-T). Which organizes into four tiers, from available today to frontier: Tier 1, now: protect and support; zinc-L-carnosine, and acid replacement (betaine HCl with pepsin) under physician supervision. This is specific to my case and not something to self-prescribe, especially given the cancer-surveillance considerations above. Tier 2, target the signaling , JAK/STAT, GSK-3, IL-17, and damp the gastrin drive (netazepide). Tier 3, reset the cells, induced regulatory T cells (iTregs). Tier 4, frontier: engineered T-cell therapy (CAR-T / CAAR-T), custom AI-designed antibodies, or synthetic proteins, that can specifically seek out inactivate or destroy the rogue immune cells attacking my stomach lining. To be clear: there's no approved cure for autoimmune gastritis today. Medicine treats it as something to manage, not solve. Tiers 2 through 4 are investigational preclinical evidence at best, and in several cases therapies that still have to be built. If you're working on autoimmune gastritis, antigen-specific tolerance, regulatory T cells, or CAAR-T for organ-specific autoimmunity, please reach out. Modern medicine has normalized too many conditions that erode our health, function, and comfort, shrinking the goal to monitoring and management while a cure is rarely even attempted. Most of these verdicts were handed down decades ago, in an era that predates nearly all of our current tech and science, and they have gone largely unchallenged. We want to change that. In the age of AI, multiomics, and custom-built DNA, proteins, and cells, no condition should be presumed incurable simply because no one has yet tried to cure it with today's stack. I’ll end on a personal note. We fill our days mostly on things that are trivial next to what we ultimately care about. We know, deep down, however, that in the noise of it all, health is easily forgotten until it’s the only thing that matters. We spend a fraction of our lives truly sober to the preciousness of life. We feel it when someone we love dies, when a child is born, when we come close to death ourselves, or when a diagnosis marks our limit. In those moments, we are sobered, and the rarity of it all becomes self evident. Imagine the existence we’d build together if that clarity didn’t fade. I wish all of you the very best. Care for yourself, care for others, care for the planet and care for our animal friends. Care for life as it’s the most precious gift there is.

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Guy
Guy@GuyDeGrove·
@RogerSeheult It’s like Europe’s absurd AC bans/limits. Only hurts yourself, coming to America soon. Bring hearths back to homes and they’d outlaw fire
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Roger Seheult, MD
Roger Seheult, MD@RogerSeheult·
There is no other US legislation pending to go into effect that could have more effect on human beings than this one. If you are looking for a hill: here it is...
Roger Seheult, MD@RogerSeheult

🚨🚨🚨We may be less than two years away from losing access to some of the most biologically useful forms of indoor lighting in the United States. On July 25, 2028, the Department of Energy’s 125 lumens-per-watt standard for General Service Lamps is scheduled to take full effect. From that date forward, covered light bulbs manufactured in or imported into the United States will have to meet that efficiency threshold. The problem is that lumens measure visible brightness—not biological usefulness. A bulb designed to provide a broad, sunlight-like spectrum, support circadian physiology, reduce blue light exposure in the evening, or emit near-infrared wavelengths may use energy in ways that are not fully reflected in its lumen rating. Near-infrared light, for example, is invisible to the human eye and therefore contributes no lumens, even though it may have important biological effects. In practical terms, the 125-lumen-per-watt rule could eliminate many circadian, broad-spectrum, and infrared-emitting bulbs from the American market. On April 8, 2025, a formal Petition for Rulemaking was submitted to the DOE requesting the creation of a new “General Wellness Lamp” product class. These lamps would be exempt from the 125-lumen-per-watt requirement while still meeting the 45-lumen-per-watt congressional backstop—representing approximately 75% lower energy use than traditional incandescent lighting. There have been encouraging political signals supporting consumer choice in lighting. However, executive orders and departmental policy statements do not, by themselves, change the Code of Federal Regulations. The 125-lumen-per-watt rule remains legally binding, with a compliance date of July 25, 2028. There is currently no waiver protecting general-wellness lighting. Proposed legislation that would repeal the rule has not passed. A durable solution requires the DOE to complete a formal rulemaking that creates a legally recognized General Wellness Lamp category. This is becoming urgent. A typical federal rulemaking may take 18 to 24 months. For a final rule to be completed with a reasonable margin before July 2028, the DOE would need to begin the formal process very soon. This should not be framed as a choice between energy efficiency and health. We should be able to preserve efficient lighting while also recognizing that light is more than visual illumination. Its spectrum, timing, intensity, and wavelength composition can affect circadian rhythms, sleep, alertness, metabolism, and potentially mitochondrial biology. Researchers, clinicians, manufacturers, and members of the public who care about healthy lighting should begin paying attention to this issue now. We need coordinated engagement with the DOE, Congress, the scientific and medical communities, and the public before the regulatory window closes. We should not allow a standard based solely on visible lumens to unintentionally remove lighting designed around human biology. @SecretaryWright @realDonaldTrump @HHSGov @RobertKennedyJr youtu.be/0m1Qekrfs7w?si…

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