纤维蛋白原与经凝乳胰蛋白酶预处理或ADP或凝血酶聚集的人血小板的关联:一项免疫细胞化学研究。

H Suzuki, R L Kinlough-Rathbone, M A Packham, H Yamazaki, J F Mustard
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引用次数: 0

摘要

尽管在没有外部纤维蛋白原的情况下,血小板也可以被诱导聚集,但纤维蛋白原大大增强了这种反应,并且纤维蛋白原与受刺激的血小板表面相关。我们比较了纤维蛋白原与ADP或凝血酶聚集的血小板表面和经凝乳胰蛋白酶处理的纤维蛋白原聚集的血小板表面的聚集反应和关联。利用电镜免疫细胞化学方法观察纤维蛋白原与血小板表面的关系。所研究的三种激动剂的聚集反应和纤维蛋白原关联模式各不相同。adp诱导的聚集与假足形成和纤维蛋白原结合有关;颗粒不释放,聚集和纤维蛋白原结合是可逆的。凝血酶诱导的聚集与广泛的假足形成和颗粒内容物的释放有关,但血小板与血小板的粘附似乎不涉及纤维蛋白原在远离颗粒排出区域的部位结合;在没有添加纤维蛋白原的情况下,没有发生分解,可见纤维蛋白也没有迅速形成。纤维蛋白原诱导的凝乳胰蛋白酶处理的血小板聚集/凝集与adp诱导的聚集相似,需要纤维蛋白原结合,颗粒内容物不释放;与adp诱导的聚集不同,adp诱导的聚集不形成假足,聚集是不可逆的。除不可逆性外,纤维蛋白原诱导的凝乳胰蛋白酶处理的血小板聚集与凝血酶诱导的未处理的血小板聚集在各方面都不同。因此,假足形成、纤维蛋白原结合和颗粒内容物的释放都不是血小板与血小板粘附的必要条件,尽管其中一个或另一个或全部可能与血小板粘附相关。如果不刺激血小板释放其颗粒内容物,纤维蛋白原结合似乎是广泛的血小板聚集所必需的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Association of fibrinogen with human platelets pretreated with chymotrypsin or aggregated with ADP or thrombin: an immunocytochemical study.

Although platelets can be induced to aggregate in the absence of external fibrinogen, the response is greatly potentiated by fibrinogen and fibrinogen becomes associated with the surface of stimulated platelets. We compared the aggregation response and association of fibrinogen with the surface of platelets aggregated by ADP or thrombin, and of chymotrypsin-treated platelets aggregated by fibrinogen. The association of fibrinogen with the surface of the platelets was visualized using an electron microscope immunocytochemical method. The aggregation response and the pattern of fibrinogen association was different with each of the three agonists studied. ADP-induced aggregation was associated with pseudopod formation and fibrinogen binding; granule contents were not released and aggregation and fibrinogen binding were reversible. Thrombin-induced aggregation was associated with extensive pseudopod formation and the release of granule contents, but platelet-to-platelet adherence did not appear to involve fibrinogen binding at sites remote from regions of granule discharge; disaggregation did not occur, and visible fibrin did not form rapidly in the absence of added fibrinogen. Fibrinogen-induced aggregation/agglutination of chymotrypsin-treated platelets was similar to ADP-induced aggregation in that fibrinogen binding was required and granule contents were not released; it differed from ADP-induced aggregation in that pseudopod formation did not occur and the aggregates were irreversible. Fibrinogen-induced aggregation of chymotrypsin-treated platelets differed from thrombin-induced aggregation of untreated platelets in every respect except irreversibility. Thus neither pseudopod formation, fibrinogen binding nor the release of granule contents is essential for platelet-to-platelet adherence, although one or other or all may occur in association with it. If platelets are not stimulated to release their granule contents, fibrinogen binding appears to be necessary for extensive platelet aggregation.

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