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NPC2蛋白的结构与功能。

Structure and function of the NPC2 protein.

作者信息

Vanier Marie T, Millat Gilles

机构信息

INSERM Unit 189, Lyon-Sud Medical School and Fondation Gillet-Mérieux, Lyon-Sud University Hospital, 69495- Pierre-Bénite Cedex, France.

出版信息

Biochim Biophys Acta. 2004 Oct 11;1685(1-3):14-21. doi: 10.1016/j.bbalip.2004.08.007.

Abstract

Somatic cell hydridization and linkage studies indicated the implication of a second gene as a cause of Niemann-Pick C disease in a minority (5%) of patients. A study of the lysosomal proteome led to the identification of a previously known gene, HE1, as the NPC2 gene. The mature NPC2/HE1 protein is a ubiquitous soluble small 132-amino-acid glycoprotein, first characterized as a major secretory protein in the human epididymis, but also detected in most tissues. Seventeen families with mutations in the NPC2 gene are known. Good genotype-phenotype correlations were observed. No distinction can be made between the biochemical phenotypes of NPC1 or NPC2 mutants. The NPC2 protein binds cholesterol with submicromolar affinity at neutral and acidic pH. The bovine protein has been crystallized, and the cholesterol-binding site assigned to a hydrophobic loosely packed region. There is strong evidence that the NPC1 and NPC2 proteins must function in a closely related fashion. Current data have led to the hypothesis that NPC2 would bind cholesterol from internal lysosomal membranes, enabling a physical interaction with NPC1 (or another protein) and allowing postlysosomal export of cholesterol. In this model, the activity of NPC1 would depend on that of NPC2. The precise function of the NPC2 protein has, however, not been fully elucidated.

摘要

体细胞杂交和连锁研究表明,少数(5%)尼曼-皮克C病患者的病因涉及第二个基因。一项对溶酶体蛋白质组的研究导致鉴定出一个先前已知的基因HE1,即NPC2基因。成熟的NPC2/HE1蛋白是一种普遍存在的可溶性小132氨基酸糖蛋白,最初被鉴定为人类附睾中的一种主要分泌蛋白,但在大多数组织中也能检测到。已知有17个家庭的NPC2基因发生了突变。观察到了良好的基因型-表型相关性。NPC1或NPC2突变体的生化表型之间无法区分。NPC2蛋白在中性和酸性pH值下以亚微摩尔亲和力结合胆固醇。牛的该蛋白已结晶,胆固醇结合位点被确定为一个疏水的松散堆积区域。有强有力的证据表明,NPC1和NPC2蛋白必须以密切相关的方式发挥作用。目前的数据导致了这样一种假设,即NPC2会结合来自溶酶体内膜的胆固醇,与NPC1(或另一种蛋白)进行物理相互作用,并允许胆固醇在溶酶体后进行输出。在这个模型中,NPC-1的活性将取决于NPC2的活性。然而,NPC2蛋白的确切功能尚未完全阐明。

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