Decreases in circulating ANGPTL3/8 concentrations following retatrutide treatment parallel reductions in serum lipids.
Wen. Yi Y; Lemen. Deven D; Lin. Yanzhu Y; Chen. Yan Q YQ; Regmi. Ajit A; Roell. William C WC; Thomas. Melissa K MK; Hartman. Mark L ML; Coskun. Tamer T; Milicevic. Zvonko Z; Haupt. Axel A; Ruotolo. Giacomo G; Konrad. Robert J RJ
Key Findings
- Retatrutide reduced circulating ANGPTL3/8 levels in both diabetic and non‑diabetic overweight participants.
- Reductions in ANGPTL3/8 were tightly linked to decreases in triglycerides and LDL‑C.
- Glucagon receptor activation (by glucagon or retatrutide) lowered ANGPTL3/8 secretion in human liver cells, and blocking the receptor stopped this effect.
Practical Outcomes
- For biohackers, the study suggests that drugs that activate the glucagon receptor—especially those that also hit GLP‑1 and GIP—might improve lipid profiles beyond glucose control. While retatrutide itself isn’t yet market‑available, the mechanism points to potential benefits of similar multi‑agonist peptides for lowering TG and LDL‑C. Keep an eye on upcoming trials and consider the lipid‑lowering angle when evaluating GLP‑1/GIP‑based compounds.
Summary
Retatrutide, a drug that hits three gut hormone receptors (GIP, GLP‑1, and glucagon), was shown in phase‑2 studies to lower blood fats (triglycerides and LDL cholesterol) by cutting down a protein complex called ANGPTL3/8. The drop in this protein matched the drop in the bad lipids, and lab work showed the glucagon part of the drug was key to this effect.
Abstract
The aim of this study was to determine if retatrutide, a triple agonist of glucose-dependent insulinotropic polypeptide (GIP) receptor, glucagon-like peptide 1 (GLP-1) receptor and glucagon (GCG) receptor, may lower serum triglyceride (TG) and low-density lipoprotein cholesterol (LDL-C) levels in part by decreasing circulating concentrations of the angiopoietin-like protein 3/8 complex (ANGPTL3/8). In post-hoc analyses of two phase 2 retatrutide trials, concentrations of ANGPTL3/8, ANGPTL4/8 complex (ANGPTL4/8), ANGPTL3 and ANGPTL4 were measured using dedicated immunoassays to determine percent changes from baseline. Correlations of ANGPTL protein and complex levels with lipid and metabolic parameters at baseline were analysed. Correlations of the changes in ANGPTL protein and complex levels versus the changes in lipid and metabolic parameters at study endpoints were also analysed. Direct effects of retatrutide itself, GIP, GLP-1, GCG and a GCG receptor (GCGR) antagonist antibody on ANGPTL3/8 secretion were studied in vitro using primary human hepatocytes. ANGPTL3/8 reductions were observed with 8 and 12 mg retatrutide doses in participants with type 2 diabetes, and with 1, 4, 8 and 12 mg retatrutide doses in participants with obesity or overweight but without diabetes. In both cases, ANGPTL3/8 decreases paralleled retatrutide-induced reductions in TG and LDL-C. In primary human hepatocytes, both glucagon and retatrutide decreased ANGPTL3/8 secretion, and these reductions were blocked with the GCGR antagonist antibody. Together, these results suggest that the GCGR agonism of retatrutide could lead to reduced circulating ANGPTL3/8 concentrations, which may then contribute to decreases in TG and LDL-C levels.
Study Information
pubmed
2025
2025-07-29T00:00:00.000Z
10.1111/dom.16661
44