CD36对氧化型低密度脂蛋白的摄取是通过一种不同于巨吞饮作用的肌动蛋白依赖性途径实现的。
Uptake of oxidized low density lipoprotein by CD36 occurs by an actin-dependent pathway distinct from macropinocytosis.
作者信息
Collins Richard F, Touret Nicolas, Kuwata Hirotaka, Tandon Narendra N, Grinstein Sergio, Trimble William S
机构信息
Program in Cell Biology, Hospital for Sick Children, Toronto, Ontario M5G 1X8, Canada.
出版信息
J Biol Chem. 2009 Oct 30;284(44):30288-97. doi: 10.1074/jbc.M109.045104. Epub 2009 Sep 9.
Abstract
The class B scavenger receptor CD36 has numerous ligands that include modified forms of low density lipoprotein, fibrillar amyloid, apoptotic cells, and Plasmodium falciparum-infected red blood cells, linking this molecule to atherosclerosis, Alzheimer disease, malaria, and other diseases. We studied the signaling events that follow receptor engagement and lead to CD36 and ligand internalization. We show that oxidized low density lipoprotein or antibody-induced clustering of CD36 triggers macropinocytosis and internalization of the receptor-ligand complex. Remarkably, however, CD36 internalization is independent of macropinocytosis and occurs by a novel endocytic mechanism that depends on actin, but not dynamin. This actin-driven endocytosis requires the activation Src family kinases, JNK, and Rho family GTPases, but, unlike macropinocytosis, it is not affected by inhibitors of phosphatidylinositol 3-kinase or Na/H exchange. Manipulation of this unique mode of internalization may prove helpful in the prevention and management of the wide range of diseases in which CD36 is implicated.
摘要
B类清道夫受体CD36有众多配体,包括低密度脂蛋白的修饰形式、纤维状淀粉样蛋白、凋亡细胞以及恶性疟原虫感染的红细胞,这使得该分子与动脉粥样硬化、阿尔茨海默病、疟疾及其他疾病相关联。我们研究了受体结合后导致CD36及其配体内化的信号转导事件。我们发现,氧化型低密度脂蛋白或抗体诱导的CD36聚集会触发巨胞饮作用以及受体-配体复合物的内化。然而,值得注意的是,CD36的内化不依赖于巨胞饮作用,而是通过一种依赖于肌动蛋白而非发动蛋白的新型内吞机制发生。这种由肌动蛋白驱动的内吞作用需要Src家族激酶、JNK和Rho家族GTP酶的激活,但与巨胞饮作用不同的是,它不受磷脂酰肌醇3激酶或Na/H交换抑制剂的影响。对这种独特内化模式的操控可能有助于预防和管理与CD36相关的多种疾病。
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