Engineering of an Ultralong-Acting and Nonaggregating Dual Amylin and Calcitonin Receptor Agonist with Durable Efficacy in Obesity and Diabetes
收藏Figshare2026-04-28 收录
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https://figshare.com/articles/dataset/Engineering_of_an_Ultralong-Acting_and_Nonaggregating_Dual_Amylin_and_Calcitonin_Receptor_Agonist_with_Durable_Efficacy_in_Obesity_and_Diabetes/30598218
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Synergistic activation of amylin and calcitonin receptors represents a distinct strategy for the treatment of obesity and diabetes. However, the inherent fibrillogenic aggregation propensity and short half-life pose significant challenges for their therapeutic translation. Here, we disclose the discovery and preclinical studies of TPM004, an ultralong-acting and nonaggregating dual amylin and calcitonin receptor agonist, endowed with balanced bioactivity. TPM004 displayed an extended half-life compatible with once-biweekly dosing in humans. In the DIO rat models, TPM004 produced robust and durable weight loss with preferential fat reduction while attenuating post-treatment adiposity rebound. TPM004 also demonstrated a prominent glucose-lowering efficacy and improved glucose homeostasis in the ZDF rats. Toxicology studies demonstrated broad safety margins for supratherapeutic exposures. Overall, these findings not only establish TPM004 as a novel DACRA preclinical candidate with strong translational promise but also represent a new paradigm for challenging peptide modifications through a long-acting helical stapling strategy.



