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Alternative Splicing Encodes Functional Intracellular CD59 Isoforms That Mediate Insulin Secretion and Are Down-Regulated in Diabetic Islets.

Proceedings of the National Academy of Sciences of the United States of America(2022)

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摘要
Significance This project describes the existence of previously unknown non–GPI-anchored CD59 isoforms required for insulin secretion, named CD59–IRIS-1 and CD59–IRIS-2, and finds reduced expression of CD59-IRIS isoforms in human diabetic islets, showing a link between dysregulation of IRIS isoforms and defects in insulin secretion in diabetic patients. These data open a path for future studies into CD59-IRIS expression and function in additional cell types capable of regulated secretion. Identification of additional specific CD59-IRIS binding partners within the cell could provide therapeutic targets for enhancement of insulin secretion in T2D.
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关键词
type 2 diabetes,insulin secretion,CD59,SNAREs,intracellular complement
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