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GLP1s; The Future of Metabolic Health (no, really)

Let’s get one thing straight; GLP-1s aren’t a trendy weight loss hack. They’re a breakthrough class of medications with over 20 years of research behind them, and their potential is only just starting to unfold. As of now, GLP-1 medications are FDA-approved to treat: •Type 2 Diabetes (since 2005) •Obesity (2023) •Cardiovascular disease (2024) Obstructive sleep apnea was recently approved under Wegovy for people with both obesity and OSA—and more new indications are on the horizon. We’re talking PCOS, fatty liver disease, kidney issues, even addiction. Several of these are already in phase 2 and 3 trials. (Yes, the future is now. Really.) And one medication I’ve got my eye on—and in my body—is Retatrutide, currently in phase 3 trials. It’s the next evolution in this class, targeting not just GLP-1 but GIP and glucagon receptors for a multi-pronged metabolic upgrade. I’m taking it. I’m thriving on it. And what it’s done for me goes way beyond the scale.

The (now famous) Gila monster

Gila monster hormones can regulate blood sugar very well It all started back in the early 1990s, when government researcher Dr. John Eng discovered that Gila monsters have a special hormone in their venom. The hormone is quite similar to a hunger-regulating hormone humans harbor in the small intestine, which helps control blood sugar levels. In people, it's called glucagon-like peptide-1. In Gila monsters, Eng named it exendin-4. Exendin-4 degrades more slowly than the human form of GLP-1, lasting for hours instead of minutes. That means it's a much better model for drug development, since it wouldn't be practical to take a drug dozens of times a day.At first, Eng tried to point this remarkable feature of Gila monster spit out to pharmaceutical makers and the government. He shopped his idea around at the Department of Veterans Affairs, where he worked at the time, as well as several different pharmaceutical companies, but didn't have much success. In the end, he patented the molecule in 1995, and licensed the discovery to a now-defunct biotech startup called Amylin. Amylin used Eng's Gila monster research to create a synthetic hormone, called extenatide. Extenatide was approved by the Food and Drug Administration (FDA) in 2005 to treat type 2 diabetes. It's still used by hundreds of thousands of children and adults with diabetes today. A safe obesity treatment that slows digestion and curbs cravings Extenatide was the very first GLP-1-mimicking drug. It ushered in a whole new class of diabetes medications that are arguably safer, and more effective, than previous treatments were. More recently, GLP-1s have been designed to target obesity, too. Today's GLP-1s work to help people lose weight because they mimic a hormone our small intestine makes naturally, which regulates hunger in several different key ways. When a patient's blood sugar levels are high, GLP-1 drugs send signals to their pancreas to secrete more insulin — but the hormone-mimicking doesn't stop there. GLP-1s also send signals to a person's brain, telling their body to feel fuller with less food. Finally, GLP-1s slow down digestion, changing the way a person's body turns food into energy. Originally, patients had to take extenatide twice a day. But, over time, newer, more advanced GLP-1s have come to market, with even longer release times (no offense, Gila monsters). Today, most GLP-1s are injected once a day, or just once a week. But they arguably wouldn't be here if it wasn't for Eng's work — which created the very first GLP-1 drug. In a statement to Insider, Novo Nordisk, the company that makes Wegovy and Ozempic, said that Gila monsters and the discovery of exendin-4 "did not have anything to do with our decision to develop long-acting GLP-1 receptor agonists" for obesity, because "that was based on GLP-1 biology in humans." But the company also said that "the GLP-1-like effect of exendin-4" in Gila monsters was "an important contribution to the field," as it led to the development of the very first injectable drug of its kind. Eng, who worked for many years at the Bronx VA medical center, was awarded a 2013 Golden Goose award, a prize meant to honor federally-funded research that leads to major biomedical breakthroughs. And, as recently as 2018, he was still collecting some royalties on the product, according to ProPublica. Funny enough, he had never actually seen a Gila monster up close until after the drug designed to mimic Gila venom was FDA approved. "It really is a beautiful lizard," he told Diabetes in Control in 2007. "The question is, what other animal has something to teach us that can be of future value? And plants, too? We will never know their value if they are gone."

About Obesity

About obesity

Think obesity’s just about overindulgence, laziness, or poor discipline? Run out of willpower?  Think again. ​Dive into the tangled tale of how this complex condition earned its disease status, who’s behind the verdict, and why it matters more than your bathroom scale ever told you. The 'old ideas' about calories in & energy out... it's NOT a thing. Turns out we are much more complex.

diet culture fail

Diet Culture Fail

Ever feel like your stomach and brain are in a toxic relationship? Blame the busted communication lines. Traditional diets set you up to fail by ignoring this glitch. Enter GLP-1: the mediator that mends the mess, so food stops ghosting your sanity. More about this gut -brain communication.

Insulin resistance 

Insulin Resistance

The Slippery Slope from Pre-Diabetes to Type 3 Diabetes (Alzheimer's) “Think your sweet tooth’s just a harmless craving? Think again. We have a LOT to Relearn. Insulin resistance is the sneaky saboteur escorting you from pre-diabetes to full-blown type 3 diabetes (yes, that’s Alzheimer’s knocking). Time to expose this metabolic mischief-maker.

The Real Dangers of Obesity

The real dangers of obesity

Sitting pretty and ignoring obesity? I get it, you are busy, over the whole thing and skeptical anyway.  Fiend, That’s kinda like rearranging deck chairs on the Titanic. With skyrocketing risks of heart disease, 17 types of cancer, and more, inaction isn’t just lazy—it’s lethal.

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