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首页> 外文期刊>Nature Communications >Lysosomal integral membrane protein-2 (LIMP-2/SCARB2) is involved in lysosomal cholesterol export
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Lysosomal integral membrane protein-2 (LIMP-2/SCARB2) is involved in lysosomal cholesterol export

机译:溶酶体整体膜蛋白-2(LIMP-2 /围巾2)参与溶酶体胆固醇出口

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The intracellular transport of cholesterol is subject to tight regulation. The structure of the lysosomal integral membrane protein type 2 (LIMP-2, also known as SCARB2) reveals a large cavity that traverses the molecule and resembles the cavity in SR-B1 that mediates lipid transfer. The detection of cholesterol within the LIMP-2 structure and the formation of cholesterolsup-/suplike inclusions in LIMP-2 knockout mice suggested the possibility that LIMP2 transports cholesterol in lysosomes. We present results of molecular modeling, crosslinking studies, microscale thermophoresis and cell-based assays that support a role of LIMP-2 in cholesterol transport. We show that the cavity in the luminal domain of LIMP-2 can bind and deliver exogenous cholesterol to the lysosomal membrane and later to lipid droplets. Depletion of LIMP-2 alters SREBP-2-mediated cholesterol regulation, as well as LDL-receptor levels. Our data indicate that LIMP-2 operates in parallel with Niemann Pick (NPC)-proteins, mediating a slower mode of lysosomal cholesterol export.
机译:胆固醇的细胞内运输受到紧张的调节。溶酶体整体膜蛋白2型(LIMP-2,也称为疤痕2)的结构揭示了横穿分子的大腔,并类似于介导脂质转移的SR-B1中的腔体。在LIMP-2结构中检测胆固醇和LIMP-2敲除小鼠中的夹杂物的形成胆固醇 - 提出了Limp2在溶酶体中转运胆固醇的可能性。我们呈现分子建模,交联研究,微观致密疗法和基于细胞的测定的结果,该测定支持胆固醇转运中的LiMP-2的作用。我们表明LIMP-2的腔结构域中的腔可以将外源胆固醇与脂液滴中的外源胆固醇粘合并递送至脂液滴。 LIMP-2的耗尽改变了SREBP-2介导的胆固醇调节,以及LDL-受体水平。我们的数据表明,LIMP-2与Niemann Pick(NPC) - 蛋白质平行进行,介导较慢的溶酶体胆固醇出口模式。

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