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囊性纤维化跨膜传导调节因子核苷酸结合结构域的纯化、特性鉴定及表达

Purification, characterization, and expression of CFTR nucleotide-binding domains.

作者信息

Clancy J P, Bebök Z, Sorscher E J

机构信息

Gregory Fleming James Cystic Fibrosis Research Center, University of Alabama at Birmingham, USA.

出版信息

J Bioenerg Biomembr. 1997 Oct;29(5):475-82. doi: 10.1023/a:1022487024031.

Abstract

The nucleotide binding domains (NBDs) within CFTR were initially predicted to lie in the cell cytoplasm, and to gate anion permeability through a pore that was present in membrane spanning alpha helices of the overall polypeptide. Our studies designed to characterize CFTR suggest several important features of the isolated nucleotide binding domain. NBD-1 appears to bind nucleotides with similar affinity to the full-length CFTR protein. In solution, the domain contains a high beta sheet content and self-associates into ordered polymers with molecular mass greater than 300,000 Daltons. The domain is very lipophilic, disrupts liposomes, and readily enters the planar lipid bilayer. Clinically important mutations in the domain may disrupt the nucleotide binding capabilities of the protein, either through a direct effect on the nucleotide binding site, or through effects that influence the overall folding of the domain in vitro. Finally, after expression in human epithelial cells (including epithelial cells from a CF patient), the first nucleotide binding domain targets the plasma membrane even in the absence of other constituents of full-length CFTR and mediates anion permeability in these cells.

摘要

最初预测囊性纤维化跨膜传导调节因子(CFTR)内的核苷酸结合结构域(NBDs)位于细胞质中,并通过整个多肽跨膜α螺旋中存在的孔来控制阴离子通透性。我们旨在表征CFTR的研究揭示了分离的核苷酸结合结构域的几个重要特征。NBD-1似乎以与全长CFTR蛋白相似的亲和力结合核苷酸。在溶液中,该结构域含有高比例的β折叠,并自缔合成分子量大于300,000道尔顿的有序聚合物。该结构域具有很强的亲脂性,能破坏脂质体,并易于进入平面脂质双层。该结构域中具有临床重要性的突变可能会破坏蛋白质的核苷酸结合能力,要么是通过直接影响核苷酸结合位点,要么是通过影响该结构域在体外的整体折叠。最后,在人上皮细胞(包括来自囊性纤维化患者的上皮细胞)中表达后,即使在没有全长CFTR的其他成分的情况下,第一个核苷酸结合结构域也会靶向质膜,并介导这些细胞中的阴离子通透性。

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