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Inaugural Article: The integrity of a cholesterol-binding pocket in Niemann–Pick C2 protein is necessary to control lysosome cholesterol levels

机译:就职文章:尼曼-皮克C2蛋白中胆固醇结合口袋的完整性对于控制溶酶体胆固醇水平是必要的

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摘要

The neurodegenerative disease Niemann–Pick Type C2 (NPC2) results from mutations in the NPC2 (HE1) gene that cause abnormally high cholesterol accumulation in cells. We find that purified NPC2, a secreted soluble protein, binds cholesterol specifically with a much higher affinity (Kd = 30–50 nM) than previously reported. Genetic and biochemical studies identified single amino acid changes that prevent both cholesterol binding and the restoration of normal cholesterol levels in mutant cells. The amino acids that affect cholesterol binding surround a hydrophobic pocket in the NPC2 protein structure, identifying a candidate sterol-binding location. On the basis of evolutionary analysis and mutagenesis, three other regions of the NPC2 protein emerged as important, including one required for efficient secretion.
机译:神经退行性疾病Niemann–Pick C2型(NPC2)是由NPC2(HE1)基因突变引起的,这些突变导致细胞中异常高的胆固醇蓄积。我们发现纯化的NPC2是一种分泌的可溶性蛋白,它以比以前报道的更高的亲和力(Kd = 30-50 nM)特异性结合胆固醇。遗传和生化研究确定了单个氨基酸的变化,可以阻止胆固醇的结合和突变细胞中正常胆固醇水平的恢复。影响胆固醇结合的氨基酸围绕NPC2蛋白结构中的疏水口袋,从而确定了候选的固醇结合位置。在进化分析和诱变的基础上,NPC2蛋白的其他三个区域显得很重要,其中一个区域是有效分泌所必需的。

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