KMID : 0620920150470120003
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Experimental & Molecular Medicine 2015 Volume.47 No. 12 p.3 ~ p.3
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The pleckstrin homology domain of phospholipase D1 accelerates EGFR endocytosis by increasing the expression of the Rab5 effector, rabaptin-5
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Park Mi-Hee
Choi Kang-Yell Min Do-Sik
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Abstract
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Endocytosis is differentially regulated by hypoxia-inducible factor-1¥á (HIF-1¥á) and phospholipase D (PLD). However, the relationship between HIF-1¥á and PLD in endocytosis is unknown. HIF-1¥á is degraded through the prolyl hydroxylase (PHD)/von Hippel?Lindau (VHL) ubiquitination pathway in an oxygen-dependent manner. Here, we show that PLD1 recovers the decrease in epidermal growth factor receptor (EGFR) endocytosis induced by HIF-1¥á independent of lipase activity via the Rab5-mediated endosome fusion pathway. EGF-induced interaction of PLD1 with HIF-1¥á, PHD and VHL may contribute to EGFR endocytosis. The pleckstrin homology domain (PH) of PLD1 itself promotes degradation of HIF-1¥á, then accelerates EGFR endocytosis via upregulation of rabaptin-5 and suppresses tumor progression. These findings reveal a novel role of the PLD1-PH domain as a positive regulator of endocytosis and provide a link between PLD1 and HIF-1¥á in the EGFR endocytosis pathway.
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