Retatrutide is an experimental medicine that copies three of the body's own appetite-and-metabolism hormones at once. Where semaglutide mimics one gut hormone and tirzepatide mimics two, retatrutide adds a third — earning it the nickname the "triple G." It is still investigational: not approved, but its early human trials produced some of the largest weight-loss numbers reported for any drug of this kind.

In plain terms: it's the next rung up the incretin ladder — one more target than tirzepatide, and still being tested.

TirzepatideGIP receptorstronger engagementGLP-1 receptorweaker engagement
Fig. Tirzepatide is a single 39-residue peptide that activates two incretin receptors — GIP and GLP-1 — via one molecule (a dual agonist). Receptor-pharmacology analyses describe it as imbalanced, engaging the GIP receptor more than GLP-1. Semaglutide, by contrast, activates GLP-1 alone.

The three-receptor mechanism ("triple G")

Your gut and pancreas release hormones after meals that manage blood sugar, appetite, and how much energy you burn. Retatrutide is a single peptide engineered to switch on three of their receptors1:

  • GLP-1 — curbs appetite and helps release insulin (the target semaglutide uses).
  • GIP — a second incretin (gut) hormone that tirzepatide adds.
  • Glucagon — the new one. Activating the glucagon receptor is thought to raise energy expenditure (how many calories the body burns) and to help clear fat from the liver.

That third lever — glucagon — is the whole point. Tirzepatide is a dual agonist (GIP + GLP-1); retatrutide is a triple agonist (GIP + GLP-1 + glucagon). One more receptor.

In plain terms: semaglutide pulls one lever, tirzepatide two, retatrutide three — and the extra lever nudges the body to burn more, not just eat less.

(The figure above shows dual GIP + GLP-1 agonism, a closely related concept; retatrutide adds a third, glucagon, target on top of the two shown.)

Why once a week

Like its approved cousins, retatrutide is built to last. Its reported half-life — how long it takes for half a dose to clear — is around 6 days, long enough that a single weekly injection keeps levels in a useful range1. That is the same weekly rhythm as semaglutide (~7 days) and tirzepatide (~5 days).

What the trials actually found

Retatrutide's phase-2 results are what put it on the map. "Phase 2" means a mid-stage human trial — larger than a first safety study, but smaller than the big phase-3 trials that support approval. Note the model in each row:

TrialPeopleKey resultYear
Jastreboff et al. — phase 2 obesity1338 adults with obesityOn the highest dose (12 mg), average weight loss of about 24% over 48 weeks2023
Sanyal et al. — phase 2a MASLD298 adults with fatty liver93% of those on 12 mg reached normal liver-fat levels (under 5%)2024

In plain terms: in a mid-stage trial, the average person on the top dose lost close to a quarter of their body weight over roughly a year1 — a bigger figure than the ~15–21% seen with semaglutide and tirzepatide in their trials. And in a separate liver-focused study, the extra glucagon action appeared to strip fat from the liver in most participants2.

Keep the honesty in view: these are phase-2 results. Encouraging, human, but mid-stage — the large phase-3 trials that decide whether a drug is approved are still running.

Where it sits on the "ladder"

The incretin medicines have been climbing a ladder of targets:

  • One receptor — semaglutide (GLP-1)
  • Two receptors — tirzepatide (GIP + GLP-1)
  • Three receptors — retatrutide (GIP + GLP-1 + glucagon)

More targets have, so far, tended to mean more weight loss in trials — though also more to learn about long-term safety. See retatrutide vs tirzepatide for the head-to-head framing.

Investigational status

This is the key honesty line: retatrutide is not an approved medicine. As of 2026 it is in late-stage clinical testing (the phase-3 TRIUMPH program) and has no regulatory approval for any use. Everything known about it comes from clinical trials, not from years of real-world use. This page explains what it is and what the trials showed — not how to use it — and it takes no position on sourcing.

Latest research (2023–2026)

  • The 2023 phase-2 obesity trial remains the headline: ~24% average weight loss at 48 weeks on the top dose, the standout result that drove interest in triple agonists1.
  • A 2024 phase-2a liver trial extended the story to fatty liver (MASLD), with 93% of the top-dose group reaching normal liver fat — a signal that the glucagon arm does something distinctive2.
  • Phase-3 trials are ongoing. The larger TRIUMPH program will determine whether these mid-stage numbers hold up and whether retatrutide reaches approval. We update this section as results report.

The short version

Retatrutide is an investigational "triple G" agonist that switches on three hormone receptors — GIP, GLP-1, and glucagon — one more than tirzepatide. In phase-2 trials it produced ~24% average weight loss and cleared liver fat in most participants, but it is not approved and its phase-3 trials are still running. Educational overview only, not medical advice.