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[关于人培养癌细胞系诱导血小板聚集的研究]

[Studies on platelet aggregation induced by human cultured carcinoma cell lines].

作者信息

Niitsu Y, Mogi Y, Bannai K, Ishii B, Ishigaki S, Kumai R, Koshida Y, Kogawa K, Kohgo Y, Urushizaki I

出版信息

Gan To Kagaku Ryoho. 1984 Mar;11(3):480-6.

PMID:6322701
Abstract

Attempts were made to clarify the mechanism of platelet aggregation and to characterize the platelet aggregating material employing established human cancer cell lines. Eleven out of the nineteen human cancer cell lines investigated showed platelet aggregating activity. The existence of divalent cation was required for the platelet aggregation induced by HMV-1 tumor cells. The platelet aggregations induced by tumor cells (HMV-1, PC-10, 3LL) were not suppressed by specific thrombin inhibitor (MD-805). The platelet aggregating activities of tumor cells (HMV-1, M 7609) were diminished by treatment with trypsin but not with collagenase or neuraminidase. Aggregating activity was preserved with a preparation of membrane from these tumor cells, although it was abolished by heating(100 degrees C 15 min) or sonication. By SDS PAGE (autoradiography), membrane proteins with MW of 20,000 daltons which specifically bound to platelets were commonly found in cells with platelet aggregating activity (HMV-1, M 7609), but were absent in platelet non-aggregating cells (HGC-25). It is therefore concluded that platelet aggregation induced by human tumor cells does not require the coexistence of thrombin, but is evoked by direct interaction of platelets with aggregating proteins (MW 20,000 daltons) on the cell membrane.

摘要

人们尝试利用已建立的人类癌细胞系来阐明血小板聚集的机制,并对血小板聚集物质进行特性描述。在所研究的19种人类癌细胞系中,有11种表现出血小板聚集活性。HMV - 1肿瘤细胞诱导的血小板聚集需要二价阳离子的存在。肿瘤细胞(HMV - 1、PC - 10、3LL)诱导的血小板聚集不受特异性凝血酶抑制剂(MD - 805)的抑制。用胰蛋白酶处理肿瘤细胞(HMV - 1、M 7609)可使其血小板聚集活性降低,但用胶原酶或神经氨酸酶处理则无此效果。这些肿瘤细胞的膜制剂保留了聚集活性,不过加热(100℃ 15分钟)或超声处理会使其丧失活性。通过SDS - PAGE(放射自显影)发现,具有血小板聚集活性的细胞(HMV - 1、M 7609)中普遍存在分子量为20,000道尔顿且能与血小板特异性结合的膜蛋白,而血小板无聚集活性的细胞(HGC - 25)中则不存在这种蛋白。因此可以得出结论,人类肿瘤细胞诱导的血小板聚集不需要凝血酶的共存,而是由血小板与细胞膜上的聚集蛋白(分子量20,000道尔顿)直接相互作用所引发。

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