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转移肿瘤细胞的血小板聚集活性。IV。细胞表面修饰对凝血酶生成、血小板聚集及随后肺定植的影响。

Platelet-aggregating activities of metastasizing tumor cells. IV. Effects of cell surface modification on thrombin generation, platelet aggregation and subsequent lung colonization.

作者信息

Tohgo A, Tanaka N G, Ogawa H

出版信息

Invasion Metastasis. 1986;6(1):58-68.

PMID:3941029
Abstract

Platelet-aggregating and thrombin-generating activities of B16 and 3LL cells were inhibited by trypsin, phospholipase A2 and by heating, but not by neuraminidase. It was confirmed that the platelet aggregation effect of these cells is due to thrombin generation. The lung-colonizing ability of treated cells injected intravenously was directly proportional to the ability to generate thrombin and to aggregate platelets. These results suggest that B16 and 3LL cells aggregate platelets through thrombin generation probably via their heat-labile surface lipoprotein, and that emboli composed of platelets, fibrin, and tumor cells may aid further the metastatic process.

摘要

B16和3LL细胞的血小板聚集和凝血酶生成活性受到胰蛋白酶、磷脂酶A2以及加热的抑制,但不受神经氨酸酶的抑制。已证实这些细胞的血小板聚集作用是由于凝血酶的生成。静脉注射处理过的细胞的肺定植能力与生成凝血酶和聚集血小板的能力直接相关。这些结果表明,B16和3LL细胞可能通过其热不稳定的表面脂蛋白生成凝血酶来聚集血小板,并且由血小板、纤维蛋白和肿瘤细胞组成的栓子可能进一步促进转移过程。

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