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KTS-去整合素抑制α(1)β(1)整合素的结构要求

Structural requirements of KTS-disintegrins for inhibition of alpha(1)beta(1) integrin.

作者信息

Brown Meghan C, Eble Johannes A, Calvete Juan J, Marcinkiewicz Cezary

机构信息

Department of Biology, Center for Neurovirology, Temple University School of Medicine, Phildelphia, PA 19122, USA.

出版信息

Biochem J. 2009 Jan 1;417(1):95-101. doi: 10.1042/BJ20081403.

Abstract

Obtustatin and viperistatin represent the shortest known snake venom monomeric disintegrins. In the present study, we have produced recombinant full-length wild-type and site-directed mutants of obtustatin to assess the role of the K(21)TS(23) tripeptide and C-terminal residues for specific inhibition of the alpha(1)beta(1) integrin. Thr(22) appeared to be the most critical residue for disintegrin activity, whereas substitution of the flanking lysine or serine residues for alanine resulted in a less pronounced decrease in the anti-alpha(1)beta(1) integrin activity of the disintegrin. The triple mutant A(21)AA(23) was devoid of blocking activity towards alpha(1)beta(1) integrin-mediated cell adhesion. The potency of recombinant KTS-disintegrins also depended on the residue C-terminally adjacent to the active motif. Substitution of Leu(24) of wild-type obtustatin for an alanine residue slightly decreased the inhibitory activity of the mutant, whereas an arginine residue in this position enhanced the potency of the mutant over wild-type obtustatin by 6-fold. In addition, the replacements L38V and P40Q may account for a further 25-fold increase in alpha(1)beta(1) inhibitory potency of viperistatin over KTSR-obtustatin.

摘要

抑胰素和蝰蛇抑素是已知最短的蛇毒单体解整合素。在本研究中,我们制备了重组全长野生型抑胰素及其定点突变体,以评估K(21)TS(23)三肽和C末端残基对特异性抑制α(1)β(1)整合素的作用。苏氨酸(22)似乎是解整合素活性最关键的残基,而将其侧翼的赖氨酸或丝氨酸残基替换为丙氨酸会导致解整合素抗α(1)β(1)整合素活性的降低不太明显。三重突变体A(21)AA(23)对α(1)β(1)整合素介导的细胞黏附没有阻断活性。重组KTS-解整合素的效力还取决于活性基序C末端相邻的残基。将野生型抑胰素的亮氨酸(24)替换为丙氨酸残基会略微降低突变体的抑制活性,而该位置的精氨酸残基会使突变体的效力比野生型抑胰素增强6倍。此外,L38V和P40Q的替换可能使蝰蛇抑素对α(1)β(1)的抑制效力比KTSR-抑胰素进一步提高25倍。

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