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CD36 facilitates fatty acid uptake by dynamic palmitoylation-regulated endocytosis

Biology

CD36 facilitates fatty acid uptake by dynamic palmitoylation-regulated endocytosis

J. Hao, J. Wang, et al.

This groundbreaking research by Jian-Wei Hao and colleagues reveals how fatty acids harness caveolae-dependent CD36 internalization to enter adipocytes. The study highlights a novel palmitoylation-regulated endocytic pathway that plays a crucial role in fatty acid uptake and lipid droplet growth, offering new insights into obesity mechanisms.... show more
Abstract
Fatty acids (FAs) are essential nutrients, but how they are transported into cells remains unclear. Here, we show that FAs trigger caveolae-dependent CD36 internalization, which in turn delivers FAs into adipocytes. During the process, binding of FAs to CD36 activates its downstream kinase LYN, which phosphorylates DHHC5, the palmitoyl acyltransferase of CD36, at Tyr91 and inactivates it. CD36 then gets depalmitoylated by APT1 and recruits another tyrosine kinase SYK to phosphorylate JNK and VAVs to initiate endocytic uptake of FAs. Blocking CD36 internalization by inhibiting APT1, LYN or SYK abolishes CD36-dependent FA uptake. Restricting CD36 at either palmitoylated or depalmitoylated state eliminates its FA uptake activity, indicating an essential role of dynamic palmitoylation of CD36. Furthermore, blocking endocytosis by targeting LYN or SYK inhibits CD36-dependent lipid droplet growth in adipocytes and high-fat-diet induced weight gain in mice. Our study has uncovered a dynamic palmitoylation-regulated endocytic pathway to take up FAs.
Publisher
NATURE COMMUNICATIONS
Published On
Sep 21, 2020
Authors
Jian-Wei Hao, Juan Wang, Huiling Guo, Yin-Yue Zhao, Hui-Hui Sun, Yi-Fan Li, Xiao-Ying Lai, Ning Zhao, Xu Wang, Changchuan Xie, Lixin Hong, Xi Huang, Hong-Rui Wang, Cheng-Bin Li, Bin Liang, Shuai Chen, Tong-Jin Zhao
Tags
fatty acids
CD36 internalization
adipocytes
palmitoylation
endocytosis
lipid droplets
weight gain
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