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Acylpeptide hydrolase is a novel regulator of KRAS plasma membrane localization and function

J Cell Sci.. 2019; 
Tan L1, Cho KJ2, Kattan WE1, Garrido CM2, Zhou Y1, Neupane P3, Capon RJ3, Hancock JF4.
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摘要

The primary site for KRAS signaling is the inner leaflet of the plasma membrane (PM). We previously reported that oxanthroquinone G01 (G01) inhibited KRAS PM localization and blocked KRAS signaling. In this study, we identified acylpeptide hydrolase (APEH) as a molecular target of G01. APEH formed a stable complex with biotinylated G01, and the enzymatic activity of APEH was inhibited by G01. APEH knockdown caused profound mislocalization of KRAS and reduced clustering of KRAS that remained PM localized. APEH knockdown also disrupted the PM localization of phosphatidylserine (PtdSer), a lipid critical for KRAS PM binding and clustering. The mislocalization of KRAS was fully rescued by ectopic expression of APEH... More

关键词

Acylpeptide hydrolase; KRAS; Oxanthroquinone; Plasma membrane; Recycling endosome; Sphingomyelin metabolism