Mould A P, Humphries M J
Department of Biochemistry and Molecular Biology, School of Biological Sciences, University of Manchester, UK.
EMBO J. 1991 Dec;10(13):4089-95. doi: 10.1002/j.1460-2075.1991.tb04985.x.
The type III connecting segment of fibronectin contains two cell binding sites, represented by the peptides CS1 and CS5, that are recognized by the integrin receptor alpha 4 beta 1. Using assays measuring the spreading of A375-SM human melanoma cells, we now report that the adhesion promoting activity of a 29 kDa protease fragment of fibronectin containing the COOH-terminal heparin-binding domain (HepII), but lacking CS1 and CS5, is completely sensitive to anti-alpha 4 and anti-beta 1 antibodies, suggesting that HepII contains a third alpha 4 beta 1-binding sequence. Examination of the primary structure of HepII revealed a sequence with homology to CS1. A 19mer peptide spanning this region (designated H1) was found to support cell spreading to the same level as the 29 kDa fragment. H1-dependent adhesion was completely sensitive to anti-alpha 4 and anti-beta 1 antibodies. When soluble peptides were tested for their ability to block cell spreading on the 29 kDa fragment, a 13mer peptide comprising the central core of H1 was found to be completely inhibitory. The active region of H1 was localized to the pentapeptide IDAPS, which is homologous to LDVPS from the active site of CS1. Taken together, these results identify a novel peptide sequence in the HepII region of fibronectin that supports alpha 4 beta 1-dependent cell adhesion.
纤连蛋白的III型连接段包含两个细胞结合位点,由肽CS1和CS5代表,可被整联蛋白受体α4β1识别。通过检测A375-SM人黑色素瘤细胞铺展的实验,我们现在报告,一种含有COOH末端肝素结合域(HepII)但缺乏CS1和CS5的29 kDa纤连蛋白蛋白酶片段的黏附促进活性,对抗α4和抗β1抗体完全敏感,这表明HepII包含第三个α4β1结合序列。对HepII一级结构的研究揭示了一个与CS1具有同源性的序列。发现一个跨越该区域的19聚体肽(命名为H1)支持细胞铺展至与29 kDa片段相同的水平。H1依赖的黏附对抗α4和抗β1抗体完全敏感。当测试可溶性肽阻断细胞在29 kDa片段上铺展的能力时,发现一个包含H1中央核心的13聚体肽具有完全抑制作用。H1的活性区域定位于五肽IDAPS,它与CS1活性位点的LDVPS同源。综上所述,这些结果确定了纤连蛋白HepII区域中一个支持α4β1依赖细胞黏附的新肽序列。
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