GIP is not your friend. And why Tirzepatide is superior to Retatrutide

[trev55]

There isn't any good long term human data on these GLP-1/GIP agonist drugs, most of what we know comes from studies on rodents so I'm going to post my thoughts about why some of these drugs may be doing more harm than good, especially in lean, insulin sensitive individuals.
I'll break it into a few parts, and why Tirz is probably much safer and better over the long term than Reta.

1. GIP is not your friend.
GIP isn’t being discussed nearly as much as GLP-1 in fitness contexts, even though many of the newest incretin drugs now deliberately agonize the GIP receptor alongside GLP-1. I want to lay out why I’m not convinced this is automatically a good thing for those who aren't fat as fuck.

Before the current popularity of dual- and multi-agonist drugs — like tirzepatide and retatrutide — GIP was originally dubbed in the literature as the obesity hormone. GIP's normal physiological role after eating is to promote fat storage in adipose tissue.

In white adipose tissue, GIP signaling tends to suppress lipolysis and promote lipid storage, causing increases in white adipose fat mass under caloric excess.

There is evidence in rats that GIP shifts insulin sensitivity in a tissue specific way, reducing insulin sensitivity in muscle, liver and brown adipose tissue, and increasing insulin sensitivity in WAT.

In rodents, CNS GIP signalling has been linked to increased neuroinflammatory signalling, and reduced leptin responsiveness in appetite-regulating centers, so it is eventually de-sensitizing you to the master satiety hormone, a condition seen in obesity.

Finally GIP is described as supporting pancreatic beta-cell proliferation and survival, which is one of the reasons it’s viewed positively in diabetes treatment. However, there is also evidence that chronic overstimulation of the GIP pathway can lead to receptor desensitization and reduced effectiveness over time.

The point is that GIP's role is not a fat loss support hormone, it is a fat storage hormone which makes me question whether strong GIP agonism is helpful or actually harmful for people without existing obesity & insulin resistance.

 

[Billbo98]

Again, who am I going to believe, you guys who regurgitate information. Use crazy high dosages, can't eat or gain muscle...

Or believe this guy? I'll take my chance with the ppl going through the process, over ppl just repeating information. That's why I call you guys trolls. Or, you're a bunch of Reddit "hot shots".. Lol

*edit* It's not bias, because they are using the exact same drug we are talking about. TF, talk about insane amounts of cope. Again, Big Paul said he was experiment also. I've said that guys will experiment and report.

Only Idiots Lose Muscle on reta.

wtf you talking about crazy high doses? I take 2mg of Tirz a week. What you’re saying is you suck off shitfluencers because they seem to know what their doing through trial and error besides just trusting the science?

 

[Billbo98]

And, if you're going to use Big Paul. Look up what he said about reta.

My point is idgaf what big Paul or Todd Lee or any of these shutfluencer coaches say about Jack because they constantly contradict themselves. Hence my serostim example.

 

[Endeavor Fitness]

wtf you talking about crazy high doses? I take 2mg of Tirz a week. What you’re saying is you suck off shitfluencers because they seem to know what their doing through trial and error besides just trusting the science?

I said I trust ppl going through the process and showing results, over you mad soyboys with you repeating information. I treat you gals like trolls..

 

[bananafeet]

I said I trust ppl going through the process and showing results, over you mad soyboys with you repeating information. I treat you gals like trolls..

Post in thread 'Giant Semaglutide Thread (and other GLP-1 / GIP agonists)'

Post in thread 'Giant Semaglutide Thread (and other GLP-1 / GIP agonists)'

Aug 15, 2025

Interesting data:
Retatrutide (LY3437943) TFA is a triple agonist peptide of the glucagon receptor (GCGR), glucosedependent insulinotropic polypeptide receptor (GIPR), and glucagon-like peptide-1 receptor (GLP-1R). Retatrutide TFA binds human GCGR, GIPR, and GLP-1R with EC50 values of 5.79, 0.0643 and 0.775 nM, respectively. Retatrutide TFA can be used for the research of obesity.

Source:

https://www.medchemexpress.com/Targets/glp-receptor.html

The novel GIP, GLP-1, and Glucagon Triple Receptor Agonist LY3437943 Exhibits Robust Efficacy in Preclinical Models of Obesity and...

• bananafeet

• 
• 

Don't be a Gronk.

Several other gut peptides, or incretin hormones secreted by enteroendocrine cells, suppress appetite. Of these, glucagon-like peptide 1 (GLP1), derived from preproglucagon, is secreted by the L cells of the intestine that also secrete peptide YY (PYY). GLP1 and PYY are co-secreted after a meal and induce satiety.29 GLP1, when infused directly into the rat ventricle, opposes the actions of orexigenic peptides including MCH and NPY.30 Glucose-dependent insulinotropic polypeptide (GIP), formerly gastric inhibitory polypeptide, is secreted from K cells in the duodenum and proximal jejunum in response to food intake.31 The incretin effect of GIP is mainly to enhance glucose-dependent insulin release from pancreatic β-cells and thereby promote postprandial plasma glucose lowering.32 The role of GIP on central appetite regulation is not straightforward, and research has suggested that GIP receptor ligands poorly influence food intake on their own. In contrast, when combined with GLP1-receptor agonists in a single peptide, appetite suppression and weight loss are enhanced, as seen with tirzepatide (discussed later). The exact mechanism of appetite suppression resulting from dual GIP and GLP1-receptor agonism remains under debate, with studies pointing to the role of GIP in adipocyte metabolism and its effect on enhancing glucagon secretion.33 Furthermore, some studies suggest that GIP receptor antagonism rather than agonism is responsible for central appetite suppression, adding to the controversy surrounding the physiologic role GIP plays in energy homeostasis.34,35

Source: Williams endocrinology




Actions of gccr:


Bonus question: what happens to your muscle stores of glycogen when you take Retatrutide?

 

[Billbo98]

I said I trust ppl going through the process and showing results, over you mad soyboys with you repeating information. I treat you gals like trolls..

Lmao soyboys are the ones suckin off influencers brotha! Good luck with that

 

[bananafeet]

I said I trust ppl going through the process and showing results, over you mad soyboys with you repeating information. I treat you gals like trolls..

@Ghoul has covered all this before. My first time reading these posts.

I wanted to see if we agreed.

Post in thread 'Stacking GLP's'

Post in thread 'Stacking GLP's'

Nov 2, 2025

@tomvet93

Retatrutide depends on a precisely tuned receptor ratio, roughly GLP-1 : GIP : glucagon = 1 : 1 : 0.3 that keeps glucagon driven fuel burning balanced by incretin driven fuel storage.

This balance lets the liver make and use glucose in harmony, providing energy without needing to break down protein for fuel.

Adding tirzepatide breaks that balance.

Its GLP-1 and GIP receptor activity is several times stronger than Retatutride’s (about 2× at GLP-1 and 5× at GIP).

When both drugs are present, Tirzepatide dominates the shared receptors, so Retatrutide’s incretin (GLP/GIP)...

• Ghoul

• 

Post in thread 'Reta phase 3 results out'

Post in thread 'Reta phase 3 results out'

Dec 11, 2025

Yes I think high dose Reta is not a great option for the general population who isn’t eating enough protein and not strength training. At some point with reta it seems the more you eat (especially carbs) the more weight you lose. I think the glucagon agonism is likely to lead to more LBM loss in the general population.

End of the day people should take what they tolerate and what is covered by their insurance. Personally, I prefer Reta but if Tirz was the only option that would be fine also.

Also, Glucagon is a catabolic hormone. This can be offset with sufficient protein...

• Ghoul

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[Mirage3000]

So, the question is REALLY, whether retatrutide and/or tirzepatide can be used as performance enhancing drugs beyond weightclass manipulation.... I read somewhere, maybe in this thread, cant remember, that retatrutide in some dosage increased endurance for some guy. Neither of the drugs are banned by WADA.

 

[bananafeet]

So, the question is REALLY, whether retatrutide and/or tirzepatide can be used as performance enhancing drugs beyond weightclass manipulation.... I read somewhere, maybe in this thread, cant remember, that retatrutide in some dosage increased endurance for some guy. Neither of the drugs are banned by WADA.

Blast tren and you will have your answer.

 

[Mfras]

Blast tren and you will have your answer.

I mean I blasted tren and lost no muscle in a cut. Also gained no meaningful tissue in that deficit state, and also easily lose no muscle with continued training stimulus and 160-350mg testosterone/week in the same cutting environment. Lifts are still (slowly) progressing as I get to the bottom of the 12% fat range.

I do use reta but was at 2 then 3mg for months, went up to 4 & 5 in recent months. All with almost zero noticeable hunger affect and the theoretical counterbalancing of GH sides is more important than any probably unnoticeable or at least unmeasurable amount of fat loss, especially when modulating daily calorie intake by ≈100 is such an easy and powerful lever to pull vs buying and pinning compounds…

 

[SubparMarioBro]

the GIP component will run into a tachyphylacic effect much sooner.

GIP tachyphylaxis seems to be inconsistent throughout the body with some tissues experiencing strong tachyphylaxis and a loss of effect while others do not (to the point of a loss of agonist effect). There’s research indicating that GIPRA’s may induce tachyphylaxis aggressively enough that you end up with functional antagonism and this has been speculated to explain some of the similarities in effect between GIP agonists and antagonists.

Considering your claims about the negative effects of GIPR agonism, I’m surprised you’d be worried about tachyphylaxis. If your earlier thoughts are correct (they’re underdeveloped) then functional antagonism via tachyphylaxis would be an ideal outcome!

 

[Slashxcode]

Agree, people are sleeping on tirz given the pride difference, especially if you're a super responder and just haven't tried it. Reta has an increased insomnia chance since it's activating.