Kisspeptin-54vsPemvidutide

Kisspeptin-54 is the full-length bioactive form of kisspeptin, cleaved from the 145-amino-acid precursor protein encoded by the KISS1 gene. It binds to KISS1R (GPR54) on GnRH neurons in the hypothalamic arcuate and anteroventral periventricular nuclei with the same binding site as KissPeptin-10 but with greater receptor affinity and a longer duration of action due to its extended peptide chain providing additional receptor contacts.

KISS1R is a Gq/11-coupled GPCR that activates phospholipase C upon kisspeptin binding, generating IP3 and DAG. IP3-mediated calcium release and DAG-activated PKC depolarize GnRH neurons, triggering robust GnRH pulse secretion into the hypophyseal portal blood supply. This GnRH pulse then stimulates anterior pituitary gonadotrophs to release both LH and FSH. The 54-amino-acid form produces a more sustained and robust GnRH/LH response compared to KissPeptin-10, attributed to its longer receptor occupancy time and potentially slower dissociation kinetics.

In clinical research, kisspeptin-54 has shown particular promise in reproductive medicine. A single bolus injection can trigger an LH surge sufficient for oocyte maturation in IVF protocols — potentially replacing the traditional HCG trigger with lower risk of ovarian hyperstimulation syndrome (OHSS), because kisspeptin's effect is physiological (triggering endogenous GnRH and LH) rather than pharmacological (directly mimicking LH like HCG). In functional hypothalamic amenorrhea (where stress or low body weight suppresses the reproductive axis), kisspeptin-54 infusion can restore LH pulsatility, confirming that the GnRH neurons remain responsive and the defect lies upstream at the kisspeptin level. The longer half-life of kisspeptin-54 compared to kisspeptin-10 (due to greater resistance to matrix metalloproteinases that degrade kisspeptins) makes it more practical for clinical applications where sustained receptor activation is desired.

Pemvidutide (ALT-801) is a once-weekly subcutaneous dual GLP-1 and glucagon receptor agonist, mechanistically similar to mazdutide and survodutide but with a distinct molecular design and a primary development focus on metabolic dysfunction-associated steatohepatitis (MASH) alongside obesity. The dual mechanism combines appetite suppression with enhanced energy expenditure and direct hepatic fat mobilisation.

The GLP-1 receptor component drives the established central appetite suppression through hypothalamic and brainstem signalling, slows gastric emptying, and stimulates glucose-dependent insulin secretion. The glucagon receptor agonism component is what differentiates pemvidutide from pure GLP-1 drugs — glucagon binding in hepatocytes activates adenylyl cyclase and protein kinase A, driving up fatty acid beta-oxidation and ketogenesis while reducing de novo lipogenesis. This directly mobilises stored hepatic triglycerides for energy use rather than continued storage, addressing the core pathology of MASH. In adipose tissue and beyond, glucagon signalling also raises whole-body energy expenditure through thermogenic and futile-cycle mechanisms.

The receptor potency ratio is balanced so that glucagon-driven hepatic glucose output is offset by GLP-1-driven insulinotropic effects, yielding net glycemic improvement alongside enhanced fat oxidation. Phase 2b results in obesity demonstrated approximately 15.6% mean body weight loss at 48 weeks, and parallel MASH trials showed significant reductions in liver fat content alongside improvements in fibrosis markers. Phase 3 trials in both obesity and MASH are now underway, positioning pemvidutide as Altimmune's lead asset and a competitor to mazdutide and survodutide in the dual GLP-1/glucagon class.