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整合素α亚基中β-螺旋桨结构域及其下表面钙结合位点的实验支持。

Experimental support for a beta-propeller domain in integrin alpha-subunits and a calcium binding site on its lower surface.

作者信息

Oxvig C, Springer T A

机构信息

Department of Pathology, The Center for Blood Research and Harvard Medical School, 200 Longwood Avenue, Boston, MA 02115, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Apr 28;95(9):4870-5. doi: 10.1073/pnas.95.9.4870.

Abstract

Integrins are large, heterodimeric surface molecules of wide importance in cell adhesion. The N-terminal half of all integrin alpha-subunits contains seven weak sequence repeats of approximately 60 amino acids that are important in ligand binding and have been predicted to fold cooperatively into a single beta-propeller domain with seven beta-sheets. We provide evidence supporting this model with a mouse mAb to human Mac-1 (alphaM beta2, CD11b/CD18). This antibody, CBRM1/20, binds to amino acid residues that are in different repeats and are 94 residues apart in the primary structure in the loop between strands 1 and 2 of beta-sheet 5 and in the loop between strands 3 and 4 of beta-sheet 6. The 1-2 loops of beta-sheets 5-7 in integrins have EF hand-like Ca2+-binding motifs. CBRM1/20 binds to Mac-1 in the presence of Ca2+ or Sr2+ with an EC50 of 0.2 mM. Mg2+ or Mn2+ cannot substitute. Antibodies to other epitopes on the Mac-1 beta-propeller domain bind in the absence of calcium. mAb CBRM1/20 does not block ligand binding. Thus, the region on the lower surface of the beta-propeller domain to which mAb CBRM1/20 binds does not bind ligand and, furthermore, cannot bind other integrin domains, such as those of the beta-subunit.

摘要

整合素是一类大型的异源二聚体表面分子,在细胞黏附中具有广泛的重要性。所有整合素α亚基的N端一半包含七个约60个氨基酸的弱序列重复,这些重复在配体结合中很重要,并且已被预测可协同折叠成一个具有七个β折叠的单一β螺旋桨结构域。我们用一种针对人Mac-1(αMβ2,CD11b/CD18)的小鼠单克隆抗体提供了支持该模型的证据。这种抗体CBRM1/20结合在不同重复序列中的氨基酸残基,这些残基在一级结构中位于β折叠5的链1和链2之间的环以及β折叠6的链3和链4之间的环中,相隔94个残基。整合素中β折叠5-7的1-2环具有EF手样Ca2+结合基序。CBRM1/20在Ca2+或Sr2+存在下与Mac-1结合,EC50为0.2 mM。Mg2+或Mn2+不能替代。针对Mac-1β螺旋桨结构域上其他表位的抗体在无钙条件下结合。单克隆抗体CBRM1/20不阻断配体结合。因此,单克隆抗体CBRM1/20结合的β螺旋桨结构域下表面区域不结合配体,而且不能结合其他整合素结构域,如β亚基的结构域。

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