Mitochondrial Peptide MOTS-c Prevents Pancreatic Cell Aging to Delay Diabetes

Mitochondria are vital organelles, crucial for cell survival and function, partly through unique peptides encoded by their own genome. While mitochondrial dysfunction is a known hallmark of age-related diseases and cellular senescence (the process of cells losing their ability to divide and function), the precise role of these mitochondrial-encoded peptides in pancreatic β-cell senescence during type 1 and type 2 diabetes pathogenesis has been largely unexplored. This study specifically addresses how the mitochondrial-encoded peptide MOTS-c influences pancreatic islet cell senescence and its potential impact on diabetes progression.

The study revealed that MOTS-c levels significantly decrease with aging and senescence in pancreatic islet cells. Treatment of aged C57BL/6 mouse pancreatic islets with MOTS-c successfully reduced pancreatic islet senescence by modulating nuclear gene expression and metabolites involved in β-cell senescence. In animal models, MOTS-c treatment improved pancreatic islet senescence and glucose intolerance in both S961-treated C57BL/6 mice and nonobese diabetic (NOD) mice. The most significant finding is that MOTS-c effectively prevents pancreatic islet cell senescence and delays the progression of diabetes in multiple mouse models. Furthermore, human data showed that circulating MOTS-c levels are notably lower in type 2 diabetes patients compared to healthy controls, suggesting a direct clinical relevance.