bd2x 🇮🇳🇺🇸

Goals set for India: By PM Modi: • Developed India by 2047 • Olympics in India by 2036 • Indian Space Station • Gaganyaan Mission • Indian on the Moon • 3rd Largest Economy • Manufacturing Superpower By Congress: • Caste Census • More Reservations • Rahul Gandhi as PM One vision asks: “How can India compete with the world?” The other asks: “How can India classify itself?” The difference is not political. It is philosophical.

Fact of the day: Pakistan shielded al-Qaeda founder Osama Bin Laden after he masterminded the 9/11 Islamic terrorist attacks that killed 3,000 Americans and prompted the War on terror. Just a couple months ago, Pakistan threatened to nuke India. In March of 2026, hundreds of Pakistani protestors shot at and firebombed the windows and gate at the US Consulate in Karachi, Pakistan and attempted to enter the building to murder US diplomats and US Marines following the death of the Supreme Leader of Iran in an air strike ordered by President Trump. The UK gang rape report just came out which shows hundreds of thousands of rapes committed against young English school girls. Guess what? All of the rapists are Pakistani Muslim men. I do not love Pakistan. It’s a disgusting Islamic country that is run by Islamic terrorist sympathizers.

TIM DAVID ABOUT HIS MIDDLE FINGER CONTROVERSY AND RCB'S TEAM ENVIRONMENT 🚨 "Honestly, I didn't want to do that, but I still haven't forgotten how I was treated in the past when I was with the Mumbai Indians. I wasn't treated properly there. In fact, during the middle of the season, I was told that I wouldn't be bought back for the next season. That's fine if you don't want to retain me, but I don't think it's right to tell a player something like that in the middle of a tournament. Even some of the owners spoke to me rudely. At one point, I seriously considered leaving the IPL midway through the season, but I convinced myself to stay and complete it. After that experience, I decided that if Mumbai Indians ever tried to sign me again, I would refuse to play for them. Now I'm with RCB, and it feels like home. The environment here is fantastic, and everyone treats me with respect. Even when I perform poorly, nobody blames me or behaves rudely. That's why I'm genuinely happy at RCB, and I would love to remain an RCBian forever."

I find it interesting that there appears to be a total media blackout & suppression pattern regarding Fauci & the recent official Tulsi Gabbard ODNI releases with new communications, emails, and notes (NOT fringe claims) challenging Fauci's sworn statements, raising serious questions on funding, COVID origins & transparency. CNN, MSNBC, ABC, CBS, NBC, NYT, & Washington Post: No prime-time segments, front-page treatments, or in-depth reporting in available searches & transcripts.

Namo Bharat RRTS is rewriting the rules of how Indian megacities move. First engineered by NCRTC, the system was designed to decongest the National Capital Region. The flagship Delhi-Ghaziabad-Meerut corridor, 82.15 km fully operational since February 2026, demonstrated the system's transformative potential. Following this success, the Parliamentary Standing Committee on Housing and Urban Affairs recommended in July 2025 that the RRTS model be expanded to other megacities facing severe congestion. The logic is simple. Indian cities are choking under migration pressure. When a town like Meerut is under 60 minutes from the capital by rapid rail, people no longer need to migrate into the city core. The RRTS system pulls commuters off congested highways onto fast, reliable networks, decongesting roads while acting as a catalyst for balanced regional development. Namo Bharat RRTS is a paradigm shift, from road-dependent, fragmented city growth to integrated, rail-anchored, multi-nodal urban development.

I'm a cardiologist. I prescribe cholesterol-lowering drugs every single day. They save lives. That science is settled and I will never tell you otherwise. But I'm going to say something that will make a lot of my colleagues uncomfortable — because someone needs to say it, and your doctor probably won't. Too many physicians make you feel crazy when you bring up statin side effects. You walk into your appointment and say "my muscles ache constantly" — and you're told it's in your head. You say "I'm exhausted all the time" — and you're told it's your age. You say "my sex drive disappeared" — and you get an awkward silence followed by a subject change. You say "I don't feel like myself anymore" — and you're told the benefits outweigh the risks, take the pill, stop reading the internet. I've watched it happen in my own field for twenty years. The conversation gets shut down. The patient gets dismissed. And then they do the one thing we should be most afraid of — they stop the medication entirely, without telling us, and lose the cardiovascular protection that's keeping them alive. That is the real cost of not being honest. Not the side effects themselves — the silence that drives patients away from treatment. In my practice, I see statin-related complications in at least 25% of my patients. Muscle pain. Fatigue that doesn't resolve with sleep. Reduced sexual drive. Brain fog. Cramping. Joint stiffness. Weakness that makes exercise — the very thing we tell them to do — feel impossible. Some of these improve with CoQ10 supplementation and optimizing vitamin D. Many do not. I wrote about the diabetes risk of statins in a New York Times op-ed in 2012. The backlash from the cardiology establishment was immediate. I was told I was undermining trust in a life-saving drug class. Fourteen years later, every major guideline acknowledges the risk I warned about. It's in the prescribing information. The physicians who attacked me for saying it now teach it to their residents. The truth doesn't care about professional comfort. It never has. Now a paper published this week in Science Advances has finally explained the mechanism behind statin myopathy — and the finding validates what millions of patients have been telling their doctors for years. Researchers discovered that statins activate the NLRP3 inflammasome in muscle cells — triggering an inflammatory cascade that causes muscle cell death, activates atrophy pathways, and disrupts muscle metabolism. This is entirely independent of the drug's cholesterol-lowering effect. The muscle damage isn't caused by lowering cholesterol. It's caused by a completely separate pharmacological action through a different pathway. The critical implication: the side effect can potentially be separated from the benefit. Blocking NLRP3 or restoring isoprenoids prevented muscle cell death without interfering with cholesterol reduction. Future therapies could preserve the cardiovascular protection while eliminating the muscle toxicity. Even more striking — the researchers found that background systemic inflammation significantly lowered the statin dose needed to trigger muscle damage. Patients with chronic inflammation, gut dysbiosis, or metabolic syndrome may be experiencing myopathy at doses their doctors consider "too low to cause problems." They're not imagining it. Their inflammatory state is priming the pathway. The muscle pain was never in their heads. It was in their NLRP3 inflammasome. And we finally have the molecular proof. Here's what I actually do in my practice — because I refuse to choose between protecting the heart and respecting the patient. Whenever possible, I avoid statins as my first-line approach for eligible patients by using alternatives that lower LDL through entirely different mechanisms with no muscle toxicity: PCSK9 inhibitors — Repatha and Praluent. Injections every 2-4 weeks that dramatically lower LDL without touching muscle tissue. No myopathy. No fatigue. No brain fog. For patients who can access them, these are transformative. Inclisiran — Leqvio. An siRNA injection I administer twice a year in my office. It silences the PCSK9 gene in the liver. Two shots a year. LDL drops roughly 50%. No muscle side effects. No daily pills. Now approved as first-line monotherapy. This is the future of lipid management and I use it aggressively. When statins ARE clinically necessary — and sometimes they are, especially post-heart attack or in combination therapy — I choose hydrophilic statins like rosuvastatin or pravastatin. These do not easily cross the blood-brain barrier. The cognitive complaints — the fog, the memory issues, the feeling of "not being yourself" — are substantially less common with these formulations because the drug stays out of the central nervous system. I never prescribe a statin without CoQ10. 100-300mg daily. Statins deplete the cellular energy molecule your muscles and heart depend on. Replenishing it reduces muscle symptoms in many patients. It should be standard practice. The fact that it isn't is a failure of our field. I check vitamin D and optimize it aggressively. Low vitamin D — which is epidemic — worsens muscle symptoms independently and compounds whatever the statin is doing. Target 50-80 ng/mL, not the bare minimum of 30. Bempedoic acid — Nexletol — for patients who can't tolerate any statin. Works upstream in the cholesterol pathway and is not active in muscle tissue. Specifically designed to avoid myopathy. Ezetimibe added to a lower statin dose. Cut the statin intensity, add ezetimibe to maintain the LDL reduction, and halve the muscle exposure. There is no excuse in 2026 for telling a patient "just deal with the muscle pain." The toolbox is deep. The alternatives exist. The only barrier is a physician's willingness to listen and adapt. I want to speak directly to every patient who has been dismissed. Your muscle pain is real. Your fatigue is real. Your cognitive changes are real. Your loss of drive — in every sense of the word — is real. A paper in Science Advances just proved the mechanism. You were never crazy. You were experiencing a documented inflammatory response in your muscle tissue that your doctor didn't have the science to explain — until this week. And I want to speak directly to my colleagues. We have to be honest. Not just about the benefits — which are enormous and undeniable — but about the side effects, the mechanism, and the alternatives. Patients who feel heard stay on treatment. Patients who feel dismissed stop their medications in silence — and die from the heart attacks we could have prevented if we'd simply been willing to have an honest conversation and switch the approach. The cardiologist who tells you statins are flawless is not protecting you. The wellness influencer who tells you statins are poison is not protecting you either. The truth lives in the middle — where it always has. Statins save lives. The side effects are real. The mechanism is now proven. The alternatives exist. And you deserve a doctor who holds all four of those truths at the same time. Both things can be true. They always could. Now we have the science to prove it.

I'm a cardiologist. Something just happened today that I genuinely did not see coming — and it could change the future of preventive medicine more than anything I've written about on this platform. Midjourney — the AI company that became famous for generating images from text prompts — just announced a medical hardware division and unveiled a working prototype of a full-body scanner unlike anything that's ever existed. It's called the Midjourney Scanner. And it works like this. You step into a shallow pool of water. You stand on a platform that slowly descends — about two inches per second — through a ring containing roughly half a million tiny ultrasonic transducers, each the size of a grain of sand. Every one of them acts as both a speaker and a microphone, sending ultrasonic waves through your body from every angle and recording what comes back. 60 seconds later, you step out. The scan is done. No radiation. No magnets. No claustrophobia. No IV contrast. Just sound, water, and an almost incomprehensible amount of computing power — roughly 2 petaflops processing 17 gigabytes per second of raw acoustic data — reconstructing a 3D map of your entire internal anatomy down to half a millimeter resolution. Organs. Tissues. Blood vessels. Bones. Muscle. Fat distribution. All segmented by AI in real time. As a cardiologist who has spent months writing about how the standard screening playbook misses the majority of future heart attacks — this is the technology I've been waiting for without knowing it existed. Here's why this matters for the future of your heart. Right now, getting a detailed look inside your cardiovascular system requires either a CT scan (radiation), an MRI (magnets, claustrophobia, 45-60 minutes, $1,000+), or a coronary CT angiogram (radiation, IV contrast, limited availability). These are powerful tools. I order them regularly and they save lives. But they're reactive. You get them when something is already suspected. They're expensive. They're uncomfortable. And for most people, they happen once — maybe twice — in a lifetime. Imagine instead: a 60-second scan with no radiation that you could repeat monthly or quarterly. Tracking cardiac structure over time. Watching body composition shift. Detecting changes in organ size, fluid distribution, or vascular architecture before symptoms ever develop. Building a longitudinal dataset of YOUR body that AI can analyze for patterns no single snapshot would reveal. That's what Midjourney is building toward. The company plans 50,000 scanners worldwide over six years, with capacity for a billion scans per month. The first location — the "Midjourney Spa" in San Francisco — opens at the end of 2027 with 10 scanners alongside saunas, cold plunges, and a gym. The scan costs a few dollars. The experience is designed to feel like wellness, not medicine. The technology is built on Butterfly Network's ultrasound-on-chip platform — 40 modules per scanner — combined with Midjourney's own AI segmentation and reconstruction stack. David Holz, the founder, claims the system aims for image quality comparable to MRI in many aspects but at nearly 100x the speed with zero radiation. Now the caveats — because I'm a physician and the caveats matter enormously. This is a Gen 1 prototype. About a dozen people have been scanned so far. Current scan time is actually closer to 20 minutes, not 60 seconds — the system is bottlenecked by bandwidth and reconstruction algorithms. The 60-second target is aspirational for future hardware generations. It is not FDA-cleared for diagnostic use. Midjourney is starting with body composition maps — a category below diagnostic imaging in the regulatory hierarchy. The path from "beautiful 3D body scans" to "clinically validated diagnostic tool that your cardiologist can act on" runs through years of clinical trials, comparative studies against MRI and CT gold standards, and FDA review. No independent clinical validation has been published. The imaging claims come from Midjourney's own demonstrations. Comparative data against established modalities does not yet exist. And the privacy implications of full-body internal scans at planetary scale — a billion scans per month — is a conversation that hasn't even started yet. So I want to be precise. This is not ready for clinical medicine today. It may not be ready for years. Many ambitious medical hardware projects have failed in the gap between prototype and product. But. The fact that a working prototype exists — producing real segmented 3D anatomy from sound waves and compute alone — means the physics works. The engineering works. The question is no longer "is this possible" but "how fast can it be validated and scaled." And if it is validated — if the resolution holds up against MRI, if the AI segmentation proves reliable, if the regulatory path clears — then what we're looking at is the most significant new imaging modality in 50 years. For my entire career, preventive cardiology has been limited by the fact that seeing inside the body is expensive, slow, uncomfortable, and infrequent. We catch disease late because we image rarely. We image rarely because imaging is hard. A 60-second, no-radiation, spa-based full-body scan that costs a few dollars would demolish every one of those barriers. I've written about AI detecting inflamed arteries. About gene editing curing cholesterol. About GLP-1 drugs rewriting metabolic medicine. About cellular reprogramming reversing aging. This is the missing piece: the ability to see inside every human body, routinely, safely, and affordably — so all of those interventions can be deployed before the disease arrives instead of after. The company that taught AI to generate images from imagination just built a machine that generates images from the human body. The future of medicine showed up today from the last place anyone expected.

The usual lies, easily disprovable. Yes, there was a cyclone, yes there was a Rice Brown spot disease lowering rice yields but that is where the truth stops. The claim that Japanese shipping prevented shipping and thus from aid reaching Bengal is a lie. Ships from Australia passed next to Ceylon. Rice could have been offloaded in Madras port and then moved by rail if needed. Yet Churchill INSISTED that this rice would not be diverted to India but sent to Greece instead. Wavell requested 1 mn tonnes of Australian Wheat. Churchill vetoed this request for the first 2 months by which time 100's of thousands were already dead. He then greenlit 200,000 tonnes of the 1 mn tonnes requested. This arrived...far too little, far too late. Canada offered 100,000 tonnes of wheat but the British govt refused this aid. The Indian assembly prepared an appeal to the United Nations Relief and Rehabilitation Administration in Dec 43, the British govt vetoed this also. "Winston may be right in saying that the starvation of anyhow under-fed Bengalis is less serious than sturdy Greeks, but he makes no sufficient allowance for the sense of Empire responsibility in this country." - Leopold Amery "“Apparently it is more important to save the Greeks and liberated countries than the Indians and there is reluctance either to provide shipping or to reduce stalks in this country.”" Sir Wavel. Clearly, Churchill considered Indians subhuman and diverted resources to Europe away from Indians. The Raj prioritised the 1 mn civilian and military workers + soldiers based in Kolkata which then produced 40% of Indias war related output. So food was there, but not for everyone. Scorched Earth - In Nov 42, months before the famine set in, the Raj enforced a brutal seizure process. All foodstocks were seized and either stockpiled under control of the military or destroyed. Fishing boats were seized (thus fish, a viable alternative in this riverine and coastal state went off the menu). This also prevented the movement of rice from usually rice surplus districts (Midnapore, Khulna and Bakarganj) not that it mattered because the Raj destroyed physical excess rice stocks in these districts. This whole scorched earth process was overseen by L G Pinell (Director Civil Supplies India). Rice output failed on account of the storm and rice disease - Half truth. Output dropped only 5% relative to 1942 but was 13% higher than 1941 and 16% higher than 1939. These years had no famine despite crop yields being far lower. Bihar, Assam and Odisha all had surplus yields of rice as well, thereby proper reallocation would have ensured that there was no famine in Bengal. States further away including Punjab also had a surplus, so overall India produced a vast surplus in 1943 that instead of feeding Bengal was exported to the UK to create a strategic stockpile of close to 18 mn tonnes of grains by the end of 1943. Bengali rice itself was being exported to Ceylon. "Mindful of our difficulties about food I told [Fazlul Huq] that he simply must produce more rice out of Bengal for Ceylon even if Bengal itself went short" Lord Linlithgow When the Bengal govt sent urgent memos to London, begging for food aid, the head of Bengal Dept of civil services was told by his bosses, "This shortage is a thing entirely of your own imagination. We do not believe it and you have got to get it out of your head that Bengal is deficit" The famine was entirely the fault of the genocidal policies of Churchill and Churchill alone.