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碱性成纤维细胞生长因子的受体结合域和肝素结合域

Receptor- and heparin-binding domains of basic fibroblast growth factor.

作者信息

Baird A, Schubert D, Ling N, Guillemin R

机构信息

Laboratories for Neuroendocrinology, Salk Institute, La Jolla, CA 92037.

出版信息

Proc Natl Acad Sci U S A. 1988 Apr;85(7):2324-8. doi: 10.1073/pnas.85.7.2324.

Abstract

Two functional domains in the primary structure of basic fibroblast growth factor (FGF) have been identified on the basis of their ability to interact with the FGF receptor, bind radiolabeled heparin, and modulate the cellular response to FGF. Peptides derived from these two functional domains can act as partial agonists and antagonists in biological assays of FGF activity. Peptides related to the sequences of FGF-(24-68)-NH2 and FGF-(106-115)-NH2 inhibit thymidine incorporation into 3T3 fibroblasts when they are stimulated by FGF but have no effect when the cells are treated with either platelet-derived growth factor or epidermal growth factor. They also possess partial agonist activity and can stimulate DNA synthesis when tested in the absence of exogenous FGF. The active peptides have no effect on the binding of epidermal growth factor to its receptor on A431 cells and they can modulate the effects of FGF, but not fibronectin, on endothelial cell adhesion. The results suggest the possibility of designing specific analogs of FGF that are capable of inhibiting the biological effects of FGF.

摘要

根据碱性成纤维细胞生长因子(FGF)一级结构中的两个功能域与FGF受体相互作用、结合放射性标记肝素以及调节细胞对FGF反应的能力,它们已被识别出来。源自这两个功能域的肽在FGF活性的生物学检测中可作为部分激动剂和拮抗剂。与FGF-(24 - 68)-NH2和FGF-(106 - 115)-NH2序列相关的肽,在FGF刺激3T3成纤维细胞时可抑制胸腺嘧啶核苷掺入细胞,但在用血小板衍生生长因子或表皮生长因子处理细胞时则无作用。它们还具有部分激动剂活性,在无外源性FGF的情况下进行检测时可刺激DNA合成。这些活性肽对表皮生长因子与其在A431细胞上的受体结合没有影响,并且它们可以调节FGF对内皮细胞黏附的作用,但不能调节纤连蛋白的作用。结果表明,有可能设计出能够抑制FGF生物学效应的FGF特异性类似物。

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