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Synthetic peptides from the carboxy-terminal globular domain of the A chain of laminin: their ability to promote cell adhesion and neurite outgrowth and interact with heparin and the beta 1 integrin subunit

机译:层粘连蛋白A链羧基末端球状结构域的合成肽:它们具有促进细胞粘附和神经突向外生长以及与肝素和β1整联蛋白亚基相互作用的能力

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摘要

The large carboxy-terminal globular domain (G domain; residues 2,110- 3,060) of the A chain of murine-derived laminin has been shown to promote heparin binding, cell adhesion, and neurite outgrowth. This study was conducted to define the potential sequence(s) originating from the G domain of laminin with any of these functional activities. A series of peptides were synthesized from the G domain, termed GD peptides, each approximately 20 amino acids long and containing multiple positively charged amino acids. In direct 3H-heparin binding assays, peptides GD-1 and GD-2 bound high levels of 3H-heparin, while peptides GD-3 and GD-4 bound lower levels of 3H-heparin, and GD-5 bound essentially no 3H-heparin. The binding of 3H-heparin to peptides GD-1 and GD-2 appeared to be of high affinity, since significant binding of 3H-heparin to these two peptides was still observed even when the NaCl concentration was raised to 1.0 M. Four of the peptides, GD-1, GD-2, GD- 3, and GD-4, directly promoted the adhesion and spreading of HT-1080 human fibrosarcoma cells as well as the outgrowth of neurites from chick spinal cord and dorsal root ganglia neurons. In addition, solutions of these peptides or antibodies generated against these peptides inhibited laminin-mediated HT-1080 cell adhesion. Antibodies against the beta 1 integrin subunit inhibited HT-1080 cell adhesion and neurite outgrowth on surfaces adsorbed with peptides GD-3 and GD-4. Therefore, laminin appears to have multiple, independent sequences in the G domain that serve a similar cell adhesion promoting function for different cell types. Furthermore, these results suggest that the sequences comprising peptides GD-3 and GD-4 use an integrin as a receptor, of which the beta 1 integrin subunit is a component for these various cell types.
机译:鼠源层粘连蛋白A链的大羧基末端球状结构域(G结构域; 2,110-3,060位残基)已显示出可促进肝素结合,细胞粘附和神经突生长。进行这项研究来确定源自层粘连蛋白G结构域的潜在序列,具有这些功能中的任何一种。从G结构域合成了一系列肽,称为GD肽,每个肽长约20个氨基酸,并含有多个带正电荷的氨基酸。在直接3H-肝素结合测定中,肽GD-1和GD-2结合高水平的3H-肝素,而肽GD-3和GD-4结合较低水平的3H-肝素,而GD-5基本上不结合3H-肝素。肝素。 3H-肝素与肽GD-1和GD-2的结合似乎具有很高的亲和力,因为即使将NaCl浓度提高到1.0 M,仍可观察到3H-肝素与这两个肽的显着结合。肽GD-1,GD-2,GD-3和GD-4直接促进HT-1080人纤维肉瘤细胞的黏附和扩散,以及神经突从鸡脊髓和背根神经节神经元的生长。另外,这些肽的溶液或针对这些肽产生的抗体抑制层粘连蛋白介导的HT-1080细胞粘附。针对β1整联蛋白亚基的抗体可抑制HT-1080细胞粘附并在吸附有肽GD-3和GD-4的表面上发生神经突生长。因此,层粘连蛋白似乎在G结构域中具有多个独立序列,可为不同类型的细胞提供相似的促进细胞黏附的功能。此外,这些结果表明,包含肽GD-3和GD-4的序列使用整联蛋白作为受体,其中β1整联蛋白亚基是这些各种细胞类型的组分。

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