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肿瘤细胞血小板聚集活性的表征

Characterization of the platelet-aggregating activity of tumor cells.

作者信息

Hara Y, Steiner M, Baldini M G

出版信息

Cancer Res. 1980 Apr;40(4):1217-22.

PMID:7357551
Abstract

Two lines of mouse tumor cells were shown to be capable of aggregating mouse and rabbit platelets in vitro. This process required higher Mg2+ concentrations than were needed by other commonly used platelet-aggregating agents. Platelet-aggregating activity was also found in tumor cell membrane fragments. This membrane-bound platelet-aggregating material contained protein, lipid, and carbohydrate moieties. The presence of all three appeared to be essential for stimulating platelet aggregation. Destruction of any component abolished its activity: protein by trypsin; lipid by phospholipase A2 and non-ionic detergents; and sialic acid by neuraminidase. Platelet aggregation induced by tumor cell membrane fragments was associated with a secretory release reaction. In this process, growth-promoting activity for tumor cells was also released from platelets. These results underline the importance of platelets in establishing tumor metastases.

摘要

有两行小鼠肿瘤细胞被证明能够在体外聚集小鼠和兔的血小板。该过程所需的镁离子浓度高于其他常用血小板聚集剂所需的浓度。在肿瘤细胞膜碎片中也发现了血小板聚集活性。这种膜结合的血小板聚集物质含有蛋白质、脂质和碳水化合物部分。这三种成分的存在似乎对刺激血小板聚集至关重要。任何一种成分的破坏都会使其活性丧失:胰蛋白酶破坏蛋白质;磷脂酶A2和非离子去污剂破坏脂质;神经氨酸酶破坏唾液酸。肿瘤细胞膜碎片诱导的血小板聚集与分泌释放反应有关。在此过程中,血小板还释放出对肿瘤细胞的生长促进活性。这些结果强调了血小板在建立肿瘤转移中的重要性。

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