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源自血小板反应蛋白、备解素和疟疾蛋白中常见序列的肽及肽类似物的生物活性。

Biological activities of peptides and peptide analogues derived from common sequences present in thrombospondin, properdin, and malarial proteins.

作者信息

Tuszynski G P, Rothman V L, Deutch A H, Hamilton B K, Eyal J

机构信息

Department of Medicine, Medical College of Pennsylvania, Philadelphia 19129.

出版信息

J Cell Biol. 1992 Jan;116(1):209-17. doi: 10.1083/jcb.116.1.209.

Abstract

Thrombospondin (TSP), a major platelet-secreted protein, has recently been shown to have activity in tumor cell metastasis, cell adhesion, and platelet aggregation. The type 1 repeats of TSP contain two copies of CSVTCG and one copy of CSTSCG, per each of the three polypeptide chains of TSP and show homology with peptide sequences found in a number of other proteins including properdin, malarial circumsporozoite, and a blood-stage antigen of Plasmodium falciparum. To investigate whether these common sequences functioned as a cell adhesive domain in TSP, we assessed the effect of peptides corresponding to these sequences and an antibody raised against one of these sequences, CSTSCG, in three biological assays which depend, in part, on the cell adhesive activity of TSP. These assays were TSP-dependent cell adhesion, platelet aggregation, and tumor cell metastasis. We found that a number of peptides homologous to CSVTCG promoted the adhesion of a variety of cells including mouse B16-F10 melanoma cells, inhibited platelet aggregation and tumor cell metastasis, whereas control peptides had no effect. Anti-CSTSCG, which specifically recognized TSP, inhibited TSP-dependent cell adhesion, platelet aggregation, and tumor cell metastasis, whereas control IgG had no effect. These results suggest that CSVTCG and CSTSCG present in the type I repeats function in the adhesive interactions of TSP that mediate cell adhesion, platelet aggregation, and tumor cell metastasis. Peptides, based on the structure of these repeats, may find wide application in the treatment of thrombosis and in the prevention of cancer spread.

摘要

血小板反应蛋白(TSP)是一种主要由血小板分泌的蛋白质,最近的研究表明它在肿瘤细胞转移、细胞黏附以及血小板聚集方面具有活性。TSP的1型重复序列在TSP的三条多肽链中,每条链都含有两个CSVTCG拷贝和一个CSTSCG拷贝,并且与许多其他蛋白质中的肽序列具有同源性,这些蛋白质包括备解素、疟原虫环子孢子蛋白以及恶性疟原虫的血液期抗原。为了研究这些共同序列在TSP中是否作为细胞黏附结构域发挥作用,我们在三种部分依赖于TSP细胞黏附活性的生物学检测中,评估了与这些序列对应的肽以及针对其中一个序列CSTSCG产生的抗体的作用。这些检测分别是TSP依赖的细胞黏附、血小板聚集以及肿瘤细胞转移。我们发现,许多与CSVTCG同源的肽促进了包括小鼠B16 - F10黑色素瘤细胞在内的多种细胞的黏附,抑制了血小板聚集和肿瘤细胞转移,而对照肽则没有效果。特异性识别TSP的抗CSTSCG抗体抑制了TSP依赖的细胞黏附、血小板聚集和肿瘤细胞转移,而对照IgG则没有作用。这些结果表明,I型重复序列中的CSVTCG和CSTSCG在TSP的黏附相互作用中发挥作用,介导细胞黏附、血小板聚集和肿瘤细胞转移。基于这些重复序列结构的肽可能在血栓形成的治疗以及癌症扩散的预防中得到广泛应用。

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