BefA, a microbiota-secreted membrane disrupter, disseminates to the pancreas and increases β cell mass

BefA 是一种由微生物分泌的膜破坏剂,可扩散至胰腺并增加 β 细胞质量

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作者:Jennifer Hampton Hill, Michelle Sconce Massaquoi, Emily Goers Sweeney, Elena S Wall, Philip Jahl, Rickesha Bell, Karen Kallio, Daniel Derrick, L Charles Murtaugh, Raghuveer Parthasarathy, S James Remington, June L Round, Karen Guillemin

Abstract

Microbiome dysbiosis is a feature of diabetes, but how microbial products influence insulin production is poorly understood. We report the mechanism of BefA, a microbiome-derived protein that increases proliferation of insulin-producing β cells during development in gnotobiotic zebrafish and mice. BefA disseminates systemically by multiple anatomic routes to act directly on pancreatic islets. We detail BefA's atomic structure, containing a lipid-binding SYLF domain, and demonstrate that it permeabilizes synthetic liposomes and bacterial membranes. A BefA mutant impaired in membrane disruption fails to expand β cells, whereas the pore-forming host defense protein, Reg3, stimulates β cell proliferation. Our work demonstrates that membrane permeabilization by microbiome-derived and host defense proteins is necessary and sufficient for β cell expansion during pancreas development, potentially connecting microbiome composition with diabetes risk.

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