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来自大肠杆菌脂多糖转运蛋白MsbA的LSGGQ和H基序的表征

Characterization of the LSGGQ and H motifs from the Escherichia coli lipid A transporter MsbA.

作者信息

Buchaklian Adam H, Klug Candice S

机构信息

Department of Biophysics, Medical College of Wisconsin, 8701 Watertown Plank Road, Milwaukee, Wisconsin 53226, USA.

出版信息

Biochemistry. 2006 Oct 17;45(41):12539-46. doi: 10.1021/bi060830a.

Abstract

ATP-binding cassette (ABC) transporters make up one of the largest superfamilies of proteins known and have been shown to transport substrates ranging from lipids and antibiotics to sugars and amino acids. The dysfunction of ABC transporters has been linked to human pathologies such as cystic fibrosis, hyperinsulinemia, and macular dystrophy. Several bacterial ABC transporters are also necessary for bacterial survival and transport of virulence factors in an infected host. MsbA is a 65 kDa protein that forms a functional homodimer consisting of two six-helix transmembrane domains and two approximately 250 amino acid nucleotide-binding domains (NBD). The NBDs contain several conserved regions such as the Walker A, LSGGQ, and H motif that bind directly to ATP and align it for hydrolysis. MsbA transports lipid A, its native substrate, across the inner membrane of Gram-negative bacteria. The loss or dysfunction of MsbA results in a toxic accumulation of lipid A inside the cell, leading to cell-membrane instability and cell death. Using site-directed spin labeling electron paramagnetic resonance spectroscopy, conserved motifs within the MsbA NBD have been evaluated for structure and dynamics upon substrate binding. It has been determined that the LSGGQ NBD consensus sequence is consistent with an alpha-helical conformation and that these residues maintain extensive tertiary contacts throughout hydrolysis. The dynamics of the LSGGQ and the H-motif region have been studied in the presence of ATP, ADP, and ATP plus vanadate to identify the residues that are directly affected by interactions with the substrate before, after, and during hydrolysis, respectively.

摘要

ATP结合盒(ABC)转运蛋白构成了已知的最大蛋白质超家族之一,并且已被证明能转运从脂质、抗生素到糖类和氨基酸等各种底物。ABC转运蛋白的功能障碍与诸如囊性纤维化、高胰岛素血症和黄斑营养不良等人类疾病有关。几种细菌ABC转运蛋白对于细菌在感染宿主中的存活和毒力因子的转运也是必需的。MsbA是一种65 kDa的蛋白质,它形成一个功能性同型二聚体,由两个六螺旋跨膜结构域和两个约250个氨基酸的核苷酸结合结构域(NBD)组成。NBD包含几个保守区域,如直接结合ATP并使其排列以便水解的沃克A、LSGGQ和H基序。MsbA将其天然底物脂多糖转运穿过革兰氏阴性菌的内膜。MsbA的缺失或功能障碍会导致脂多糖在细胞内的毒性积累,导致细胞膜不稳定和细胞死亡。使用定点自旋标记电子顺磁共振光谱,已对MsbA NBD内的保守基序在底物结合时的结构和动力学进行了评估。已确定LSGGQ NBD共有序列与α螺旋构象一致,并且这些残基在整个水解过程中保持广泛的三级接触。已分别在ATP、ADP以及ATP加钒酸盐存在的情况下研究了LSGGQ和H基序区域的动力学,以确定分别在水解之前、之后和过程中直接受与底物相互作用影响的残基。

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