Apr 23, 2020

BLOS1 mediates kinesin switch during endosomal recycling of LDL receptor

BioRxiv : the Preprint Server for Biology
C. ZhangWei Li

Abstract

Low-density lipoprotein receptor (LDLR) in hepatocytes plays a key role in normal clearance of circulating LDL and in whole body cholesterol homeostasis. The trafficking of LDLR is highly regulated in clathrin-dependent endocytosis, endosomal recycling and lysosomal degradation. Current studies have been focusing on its endocytosis and degradation. However, the detailed molecular and cellular mechanisms underlying its endosomal recycling are largely unknown. We found that BLOS1, a shared subunit of BLOC-1 and BORC, is involved in LDLR endosomal recycling. Loss of BLOS1 leads to less membrane LDLR and impairs LDL clearance from plasma in hepatocyte-specific BLOS1 knockout mice. BLOS1 interacts with kinesin-3, and that BLOS1 acts as a new adaptor for kinesin-2 to coordinate kinesin-3 and kinesin-2 during the long-range transport of recycling endosomes (REs) to plasma membrane along microtubule tracks to overcome hurdles at microtubule intersections. These findings provide new insights into REs anterograde transport and the pathogenesis of dyslipidemia.

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Mentioned in this Paper

Computer Software
Biological Markers
Genome
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Impacted Tooth
Genomics
Cell Growth
Sequencing
Massively-Parallel Sequencing
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