The NERP-4-SNAT2 axis regulates pancreatic β-cell maintenance and function - Université de Lille
Article Dans Une Revue Nature Communications Année : 2023

The NERP-4-SNAT2 axis regulates pancreatic β-cell maintenance and function

Résumé

Insulin secretion from pancreatic β cells is regulated by multiple stimuli, including nutrients, hormones, neuronal inputs, and local signalling. Amino acids modulate insulin secretion via amino acid transporters expressed on β cells. The granin protein VGF has dual roles in β cells: regulating secretory granule formation and functioning as a multiple peptide precursor. A VGF-derived peptide, neuroendocrine regulatory peptide-4 (NERP-4), increases Ca2+ influx in the pancreata of transgenic mice expressing apoaequorin, a Ca2+-induced bioluminescent protein complex. NERP-4 enhances glucose-stimulated insulin secretion from isolated human and mouse islets and β-cell–derived MIN6-K8 cells. NERP-4 administration reverses the impairment of β-cell maintenance and function in db/db mice by enhancing mitochondrial function and reducing metabolic stress. NERP-4 acts on sodium-coupled neutral amino acid transporter 2 (SNAT2), thereby increasing glutamine, alanine, and proline uptake into β cells and stimulating insulin secretion. SNAT2 deletion and inhibition abolish the protective effects of NERP-4 on β-cell maintenance. These findings demonstrate a novel autocrine mechanism of β-cell maintenance and function that is mediated by the peptide–amino acid transporter axis.
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hal-04709272 , version 1 (25-09-2024)

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Weidong Zhang, Ayako Miura, Md Moin Abu Saleh, Koichiro Shimizu, Yuichiro Mita, et al.. The NERP-4-SNAT2 axis regulates pancreatic β-cell maintenance and function. Nature Communications, 2023, Nature Communications, 14 (1), pp.8158. ⟨10.1038/s41467-023-43976-8⟩. ⟨hal-04709272⟩
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