I’m a Pathologist: The "Biological Cost" of Ozempic and Mounjaro.

In 2024, humanity discovered something extraordinary. [music] A weekly

extraordinary. [music] A weekly injection that could quiet hunger, stabilize blood sugar, and melt weight faster than anything medicine had seen.

Headlines called it the end of obesity, the billiondoll miracle, the cure. But

I'm a pathologist, and in my world, miracles don't really exist in this setting.

There's always mechanisms behind [music] everything. Anytime you override a

everything. Anytime you override a biological system that took 2 million years to evolve, you are making a trade.

And every trade has an invoice, a cost to pay and a receipt. Right now, the public conversation around GLP-1 medications, some of

as you may know them commercially, Ompic and Monero, is chaotic.

Half promise salvage and half warn of disaster. Very few explain the biology.

disaster. Very few explain the biology.

So today we're going to fix that. Please

feel free to leave your experience in the comments below. I read every single one. I'm Dr. Amin Haday, triple board

one. I'm Dr. Amin Haday, triple board certified pathologist, physician, [music] and a susan clinical professor.

My career is spent reading the truth written inside human cells. Cells don't

argue. Cells don't lie.

They respond to chemistry.

If clear science-based breakdowns like this help you, feel free to like this video so more people can find evidence over confusion.

This video is your evidence-based mechanism first understanding of GLP-1 drugs. How they work, why they work,

drugs. How they work, why they work, [music] why they sometimes backfire, and how to use them safely.

We'll walk through the evolutionary trap behind modern obesity, the lizard brain that controls hunger, the Gilla monster

discovery that changed medicine, the engineering behind 7-day appetite suppression, the benefits, the trade-offs, and the real world risks.

And finally, the safe medically aligned exit strategy.

This is not fear. This is not hype and it's purely physiology. If you

appreciate science explained clearly, liking and subscribing helps these videos reach more people who need clarity and not confusion. So, let's

begin. You first have to understand why losing weight is biologically difficult.

Let me start with a truth almost no one hears from their doctor. Obesity is not a moral failure. It's an evolutionary

success.

For 99.9% of human history, starvation, not overeating, was the number one cause of death.

Anthropologists writing in the Journal of Human Evolution describe how hunger shaped early human survival.

The people who could store fat the most efficiently survived. Those who burned

efficiently survived. Those who burned through calories quickly didn't.

So, you are the descendants of the world's best fat stores. Your biology is optimized to survive scarcity, but you

live in an age of abundance. Your genes

expect famine.

You're surrounded by Uber Eatats and Door Dash. And by the way, no

Door Dash. And by the way, no affiliation. This mismatch is what

affiliation. This mismatch is what evolutionary biologists call an evolutionary mismatch.

Your biology is ancient. Your

environment is new.

And this conflict makes weight loss feel like swimming against a biochemical current.

But it gets more interesting once you understand the wiring. In the deepest part of your brain lies the hypothalamus, the lizard brain, responsible for

survival temperature thirst stress and hunger.

This region defends your body fat set point with military precision. It uses

two hormones to do it. Grein, which is essentially the gas pedal, is produced by the stomach when empty. It travels up

the vagus nerve and says we need food.

This is primal overpowering and has been shown in nature reviews endocrinology to override willpower

completely. Then we have leptin which is

completely. Then we have leptin which is the break. It's produced by fat cells.

the break. It's produced by fat cells.

When stores are full, leptin tells the brain, "We have enough. Stop eating."

But here's the problem. In obesity, the brain becomes leptin resistant just like you stop smelling perfume

after a few minutes. This is why someone can have 80, 100, even 150 lbs of energy stored in their body and still feel

hungry.

This isn't weakness, it's wiring. GLP-1

medications override this broken circuit. But the discovery didn't begin

circuit. But the discovery didn't begin in a lab. It began in a desert with a venomous lizard.

In the 1980s, scientists noticed something fascinating. If you inject

something fascinating. If you inject sugar into someone's bloodstream, the insulin response is small. But if they drink the same sugar, the insulin

response is huge.

Why? Because the gut warns the body in advance.

Intestinal cells called L cells release a hormone called GLP-1.

GLP1 does three things immediately. It

prepares the pancreas for insulin. It

slows the stomach. It tells the brain we're satisfied.

This is called the incretin effect.

first described in the journal of clinical investigation. But natural

clinical investigation. But natural GLP-1 breaks down in just two minutes because of an enzyme called DPP4. If

scientists wanted to use GLP-1 as a drug, they needed to outsmart DPP4.

The breakthrough came from a creature most people have never even heard of, the Gilla Monster. In the deserts, there

is a venomous lizard that eats only a few times a year. A researcher named Dr. John Ang discovered its venom contain a

molecule called extendin 4 described in endocrinology in 1992.

Accendin 4 acts like GLP-1, binds the same receptor, but doesn't break down quickly.

It doesn't get sliced apart by DPP4.

It survives.

This was the blueprint for the first GLP-1 medications.

But modern scientists took this idea and engineered something far more powerful, a hormone that can survive for 7 days.

This is the part that blows people's minds. Smoglutide, the molecule in ompic

minds. Smoglutide, the molecule in ompic and wiggoi is a triumph of modern chemistry.

Researchers wanted something that behaved like natural GLP1 but lasted long enough to be effective as a weekly therapy.

They did two brilliant things and it was discussed in nature biology in 2017.

They changed one amino acid.

This prevents DPP4 from cutting the molecule. They attached a C18 fatty acid

molecule. They attached a C18 fatty acid tail. This tail binds to albumin which

tail. This tail binds to albumin which is a massive protein circulating in your blood for about a week. Albamin acts

like a cruise ship. Semaglutide attaches

to it and coast through your bloodstream for days. A hormone that should last

for days. A hormone that should last only 2 minutes now lasts 168 hours.

This one modification changed the landscape of metabolic medicine.

And then came the upgrade.

Terzepatite known as Monero and Zepbound doesn't activate just one receptor. It

activates two GLP1 and GIP. The dual

action was first described in the New England Journal of Medicine in 2022

comparing tzipatite to semolutide. When

combined, GLP1 quiets appetite. GIP

stabilizes nausea and enhances glucose control.

This synergy allows for deeper appetite reduction with potentially better tolerance for many patients. This is why turepite often leads to greater average

weight loss than semlutide in clinical trials though individual results vary.

We've covered the evolutionary trap, the wiring, the discovery, the engineering, and the upgrade. Now, we need to talk about the part nobody explains clearly.

The trade-offs, the risks, the physiology behind side effects. It's not

fear, not hype, just biology. GLP-1

medications work in part by slowing stomach emptying, something documented extensively in gastroenterology research, including clinical

gastroenterology and hepatology in 2023.

For many people, this effect is mild and therapeutic.

It keeps food in the stomach longer, reducing appetite. But for a subset of

reducing appetite. But for a subset of individuals, especially at higher doses, this delay can become more pronounced.

Some people experience nausea, reflex, bloating, early fullness, slower digestion. Most of the time these

digestion. Most of the time these symptoms are manageable but sometimes they improve with dose adjustment

but in rare cases the slowing can be significant enough that clinicians evaluate for delayed gastric emptying

sometimes referred to as gastroparesis.

Case reports published in GI literature describe a small number of patients developing more severe symptoms.

Bloating, vomiting, and difficulty handling solid meals. Again, it's rare, but it's real.

Not a guarantee, but important to understand.

And then there's something patients don't hear until the day of surgery, the anesthesia problem.

If your stomach empties more slowly than usual, you may have residual food in your stomach even after fasting. This

matters because anesthesia turns off the protective airway reflexes. If vomiting

occurs while sedated, stomach contents can enter the lungs. Sometimes

anesthesiologists call this aspiration.

Because of this, the American Society of Anesthesiologists in 2023 issued updated guidelines recommending special

precautions for patients on GLP-1 medications before surgery. This doesn't

mean anesthesia is unsafe, but it does mean your anesthesiologist needs to know you're on these medications. So, awareness is

medications. So, awareness is prevention.

Let's talk about the pancreas. One of

the most misunderstood topics in the GLP-1 discussion.

There have been reports of pancreatitis, which is the inflammation of the pancreas in people taking GLP-1 medications. Large clinical trials,

medications. Large clinical trials, including those published in gastroenterology in 2022, show that the overall risk appears low, but the

prescribing information include caution for a reason. People with a history of

reason. People with a history of pancreatitis, very high triglycerides, heavy alcohol use already carry a baseline risk for pancreatic

inflammation.

For these individuals, clinicians often use extra caution when considering GLP-1 drugs. Most patients will never

drugs. Most patients will never experience this issue. But if someone on these medications develops persistent severe abdominal pain, that is something

a physician should evaluate. This isn't

fear. It's simply understanding the physiology and respecting individual risk factors. Every GLP1 medication has

risk factors. Every GLP1 medication has a boxed warning related to thyroid sea cell tumors in animals. specifically

rodents.

Here's the nuance. Rodents have many GLP-1 receptors on their thyroid C cells. Humans have far fewer. This is

cells. Humans have far fewer. This is

why rodent studies showed tumors and human studies have not shown a clear increase at least so far.

This study was published in thyroid journal in 2023. However, and this is important, people with a personal or

family history of medularary thyroid cancer or the genetic condition men too are generally advised not to take these medications.

Not because we've proven harm in humans, but because we don't yet have 20-year population data.

This is what good medicine does. It

weighs uncertainty honestly and protects the people who have known genetic vulnerabilities. Muscle loss. This is

vulnerabilities. Muscle loss. This is

the most underrated biological trade-off and one that surprises almost everyone.

When you lose weight quickly from any method, you lose both fat and muscle. On

GLP-1 medications, appetite drops dramatically. Protein intake often

dramatically. Protein intake often decreases. strength training becomes

decreases. strength training becomes harder. Nausea can reduce food variety.

harder. Nausea can reduce food variety.

Emerging studies, include those in the Obesity Journal in 2023, show that without deliberate nutritional and resistant training support, some

patients lose a meaningful percentage of lean mass.

Why does this matter? Because muscle is the engine of your metabolism.

The main side of glucose disposal, a buffer against insulin resistance, a protector against falls, a predictor

of longevity. So less muscle means lower

of longevity. So less muscle means lower metabolic rate, lower metabolic rate

means easier weight gain.

This is not unavoidable, but without strategy, it is very common. This is why the protein floor and strength training,

which we'll cover in the next part, are non-negotiable. Now, let's talk about

non-negotiable. Now, let's talk about facial changes. There's a lot of buzz

facial changes. There's a lot of buzz about ompic face. Here's the truth. It's

not the drug damaging the skin. It's

rapid fat loss. When fat pads in the face shrink quickly, the skin doesn't always retract at the same pace. Plastic

surgeons and dermatologists, including those publishing in the aesthetic surgery journal in 2024, describe this as a simple volume change.

It's not a toxicity reaction. It's

physics. Slower, steadier weight loss preserves facial structure better.

Strength training and protein intake helps too.

This is a topic I hear quietly in clinics and see openly in support groups. Some people describe feeling

groups. Some people describe feeling less impulsive, less interested in food, calmer, more stable, and for many, this

is a benefit, especially those who struggle with emotional or binge eating.

But a subset describe something different. Less motivation,

different. Less motivation, less pressure, muted joy, a grayscale feeling, lower reward drive. It's not

sadness. It's not quite depression, just reduced spark. Pre-clinical

research in translational psychiatry published in 2024 and ongoing human studies suggest GLP-1 receptors in the

reward pathways including the nucleus encumbent may modulate dopamine signaling.

Not everyone, not dramatically in most, but enough for people to notice. This is

why monitoring your mental and emotional landscape is important while on these medications.

If you feel flatter than expected, your clinician probably wants to know.

Now we arrive at the question everyone asks. If I stop ompic or monero, will I

asks. If I stop ompic or monero, will I gain the weight back? The most evidence aligned answer is many people regain

weight without a strategy. Not because

they failed, because biology rebounds.

In the step one extension trial published in New England Journal of Medicine in 2022, participants regained roughly 2/3 of the weight they lost 12

months after stopping unless they had a robust lifestyle support. Here's why this happens. This

support. Here's why this happens. This

is the part nobody explains clearly.

Hunger hormones surge back. While on GLP medications, ghrein, your hunger hormone is suppressed. When the medication

is suppressed. When the medication leaves your system, ghrein doesn't return to baseline. It overshoots.

This is well documented in metabolic studies published in endocrine reviews in 2021. Number two, appetite returns

in 2021. Number two, appetite returns faster than satiety signals. the brain

stem, the hypothalamus regains sensitivity before the gut does.

That mismatch creates a transient hyper hunger period. Number three is muscle

hunger period. Number three is muscle mass has decreased. During weight loss, people often lose some lean mass. Less

muscle means a slower metabolic rate.

This is well documented in obesity journals in 2023. So when appetite

returns, the engine is smaller.

Fat reaccumulates faster than muscle.

This is a universal physiological pattern called preferential atapose regain. This was demonstrated in

regain. This was demonstrated in metabolism journal quite well in 2019.

Fat comes back quickly. Muscle rebuilds

slowly.

This combination creates what researchers call rebound physiology.

This is not about willpower. This is not about character. This is chemistry. It's

about character. This is chemistry. It's

physics. And physics can be engineered.

That brings us to the path forward, which are my protocols that are based on peer-reviewed literature. If you are on

peer-reviewed literature. If you are on GLP-1 medications now, or if you ever plan to stop, these next steps are core

of protecting your biology. Of course,

this has to happen after you speak to your personal physician.

These protocols are supported by evidence from journals like sports medicine, cell metabolism and nutrition reviews.

This is how you prevent muscle loss.

This is how you minimize rebound and land safely.

Rule number one, the protein floor. This

is a non-negotiable.

When appetite is low, protein is the first thing to disappear, but it is the last thing your body wants to lose.

Aim for adequate protein intake daily.

Your clinician should guide your specific target. If solid food feels

specific target. If solid food feels heavy, there are alternatives such as clear whey isolate, collagen and

essential amino acids, dairy proteins, and egg white proteins. Why? Because

leucine and other amino acids directly signal the muscle to stay intact.

Protein is proactively your muscle insurance and muscle is your metabolic insurance. This was shown in journal of

insurance. This was shown in journal of physiology in 2020.

Rule number two, strength training is mandatory.

There is no drug, no supplement, no hack that can replace mechanical load on muscle. Resistant training two to four

muscle. Resistant training two to four days per week is helpful. You can try

squats deadlifts rows presses pulls.

This signals your body, don't break down this tissue. We need

it.

Studies in sports medicine 2023 show that even 2 days per week of resistant training can drastically reduce lean

mass loss during weight loss. This is

not about looking fit. This is about metabolic preservation. Rule number

metabolic preservation. Rule number three, taper slowly. If you ever decide, of course, in synergy with your medical

doctor to come off GLP-1 medications, do not stop abruptly. A sudden drop in GLP1 signaling creates a rapid rebound in

appetite. A gradual taper allows hunger

appetite. A gradual taper allows hunger hormones to recalibrate, satiety signals to normalize,

your routine to strengthen, your muscles to grow, your metabolism to stabilize.

This approach is supported by clinical observations in obesity medicine practices and aligns with the physiology described in endocrinology and

metabolism clinics which was published in 2022.

Your body needs time to readjust. Give

it that time.

Rule number four is use fiber as a mechanical satiety tool. Once medication

doses decrease, your stomach begins sending hunger signals again. To bridge

this gap, use high volume, low calorie foods to stretch the stomach's mechanical receptors. You can uh try

mechanical receptors. You can uh try oats beans berries vegetables lentils, psyllium husk.

This strategy is backed by satiety research published in appetite journal in 2020.

Chemical satiety by GLP1 transitions to mechanical satiety with

fiber and volume.

This is how you hand the baton from the drug to your stomach.

Rule number five, monitor mood, motivation, and joy. GLP-1 receptors

exist in the reward pathways of the brain. Some individuals experience a

brain. Some individuals experience a calmer, quieter relationship with food, which can be beneficial,

but a smaller subset describe it muted emotional tone.

If your motivation drops, if you lose interest in hobbies, if life feels flatter, speak with your physician. Studies in translational

physician. Studies in translational psychiatry in 2024 are exploring this finding. It may be dose related,

finding. It may be dose related, transient, or it may require adjustment.

Your emotional landscape is as important as your metabolic one.

GLP-1 medications have taught us something profound. Obesity is biology,

something profound. Obesity is biology, not a moral issue. For many, these medications reduce cardiovascular risk,

improve metabolic health, stabilize blood sugar, calm obsessive food thoughts, break cycles that have lasted for

decades. For others, these drugs are a

decades. For others, these drugs are a bridge, a tool that helps them build new habits while biology stabilizes. And for

some, there are real tradeoffs that require careful navigation. There is no oneizefitsall answer.

There is only informed consent, evidence-based decisionmaking, and respect for the complexity of the human body.

You're not weak. You're not broken.

You're not a moral failure.

You're a human being living in an environment your biology was never designed for.

And now finally you have a tool, a powerful one, pair it with a protocol that honors your physiology.

Thank you for your time, your curiosity, and your commitment to understanding your body on a deeper level. Let's

continue building a life that is healthy coherent energized and uninflamed. [music]

uninflamed. [music] I'm Dr. Hayad and I'll see you in the next