MicroRNAs-103/107 coordinately regulate macropinocytosis and autophagy

Macropinocytosis, by which cells ingest large amounts of fluid, and autophagy, the lysosome-based catabolic process, involve vesicular biogenesis (early stage) and turnover (end stage). Much is known about early-stage events; however, our understanding of how the end stages of these processes are go...

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Veröffentlicht in:The Journal of cell biology 2016-12, Vol.215 (5), p.667-685
Hauptverfasser: Park, Jong Kook, Peng, Han, Katsnelson, Julia, Yang, Wending, Kaplan, Nihal, Dong, Ying, Rappoport, Joshua Z, He, CongCong, Lavker, Robert M
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Sprache:eng
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Zusammenfassung:Macropinocytosis, by which cells ingest large amounts of fluid, and autophagy, the lysosome-based catabolic process, involve vesicular biogenesis (early stage) and turnover (end stage). Much is known about early-stage events; however, our understanding of how the end stages of these processes are governed is incomplete. Here we demonstrate that the microRNA-103/107(miR-103/107) family, which is preferentially expressed in the stem cell-enriched limbal epithelium, coordinately regulates aspects of both these activities. Loss of miR-103/107 causes dysregulation of macropinocytosis with the formation of large vacuoles, primarily through up-regulation of Src, Ras, and Ankfy1. Vacuole accumulation is not a malfunction of early-stage autophagy; rather, miR-103/107 ensure proper end-stage autophagy by regulating diacylglycerol/protein kinase C and cyclin-dependent kinase 5 signaling, which enables dynamin to function in vacuole clearance. Our findings unveil a key biological function for miR-103/107 in coordinately suppressing macropinocytosis and preserving end-stage autophagy, thereby contributing to maintenance of a stem cell-enriched epithelium.
ISSN:0021-9525
1540-8140
DOI:10.1083/jcb.201604032