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嫁接到葡萄球菌蛋白A上的层粘连蛋白衍生YIGSR序列的细胞黏附活性和受体结合特异性。

Cell-adhesive activity and receptor-binding specificity of the laminin-derived YIGSR sequence grafted onto Staphylococcal protein A.

作者信息

Maeda T, Titani K, Sekiguchi K

机构信息

Research Institute, Osaka Medical Center for Maternal and Child Health.

出版信息

J Biochem. 1994 Feb;115(2):182-9. doi: 10.1093/oxfordjournals.jbchem.a124315.

DOI:10.1093/oxfordjournals.jbchem.a124315
PMID:8206865
Abstract

Laminin contains multiple oligopeptide motifs to promote cell adhesion and migration. One of these motifs is YIGSR within the B1 chain. We reconstituted the cell-adhesive activity of YIGSR motif by grafting it onto a truncated form of the Staphylococcal protein A (designated tSPA) via cassette mutagenesis. When coated on a polystyrene surface, the YIGSR-grafted tSPA (YIGSR-tSPA) promoted attachment and spreading of mouse melanoma and human rhabdomyosarcoma cells, but not of hamster fibroblasts. The cell-adhesive activity of YIGSR-tSPA was abolished by amino acid substitution or scrambling of the inserted YIGSR sequence. Divalent cations Mn2+ and Mg2+, but not Ca2+, promoted the cell adhesion to YIGSR-tSPA. Interestingly, the YIGSR-tSPA-mediated cell adhesion was barely inhibited by the linear peptide CDPGYIGSR-NH2, but was strongly inhibited by the cyclic peptide CDPGYIGSRC and another peptide PEILDVPST, which is a specific inhibitor for integrin alpha 4 beta 1. Among various anti-integrin antibodies, anti-alpha 4 and anti-beta 1 antibodies specifically inhibited the cell adhesion to YIGSR-tSPA. In support of these observations, adhesion of rhabdomyosarcoma cells to intact laminin was also partially inhibited by synthetic PEILDVPST peptide and anti-alpha 4 antibody. These results, taken together, indicate that the YIGSR motif exerts its cell-adhesive activity through interaction with integrin alpha 4 beta 1.

摘要

层粘连蛋白含有多个促进细胞黏附和迁移的寡肽基序。其中一个基序是B1链内的YIGSR。我们通过盒式诱变将YIGSR基序嫁接到葡萄球菌蛋白A的截短形式(称为tSPA)上,重建了YIGSR基序的细胞黏附活性。当包被在聚苯乙烯表面时,YIGSR嫁接的tSPA(YIGSR-tSPA)促进小鼠黑色素瘤细胞和人横纹肌肉瘤细胞的附着和铺展,但不促进仓鼠成纤维细胞的附着和铺展。插入的YIGSR序列的氨基酸取代或扰乱消除了YIGSR-tSPA的细胞黏附活性。二价阳离子Mn2+和Mg2+,而不是Ca2+,促进细胞对YIGSR-tSPA的黏附。有趣的是,YIGSR-tSPA介导的细胞黏附几乎不受线性肽CDPGYIGSR-NH2的抑制,但受到环肽CDPGYIGSRC和另一种肽PEILDVPST(整合素α4β1的特异性抑制剂)的强烈抑制。在各种抗整合素抗体中,抗α4和抗β1抗体特异性抑制细胞对YIGSR-tSPA的黏附。为支持这些观察结果,合成的PEILDVPST肽和抗α4抗体也部分抑制了横纹肌肉瘤细胞对完整层粘连蛋白的黏附。综上所述,这些结果表明YIGSR基序通过与整合素α4β1相互作用发挥其细胞黏附活性。

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