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用血小板活化因子(PAF-乙酰醚)使兔血小板脱颗粒:一种揭示血小板活化物质作用方式的新方法。

Degranulation of rabbit platelets with PAF-acether: a new procedure for unravelling the mode of action of platelet-activating substances.

作者信息

Vargaftig B B, Joseph D, Marlas G, Chevance L G

出版信息

Thromb Haemost. 1982 Aug 24;48(1):67-71.

PMID:7135345
Abstract

Aggregation and secretion of ATP induced by thrombin, collagen, the snake venom component convulxin and platelet-activating factor (PAF-acether) were studied after the exposure of rabbit platelets to 1 microM of PAF-acether. This concentration, which is around 6 orders of magnitude above the concentration needed to induce full aggregation, was required to remove most of the releasable ATP from the platelets. The depleted platelets aggregated to PAF-acether, to thrombin and to convulxin under conditions where only very low amounts of ATP were secreted, confirming that these agents do not require the release of dense body components to trigger aggregation. Furthermore, when exposure to PAF-acether was associated to inactivation of platelet cyclooxygenase with aspirin, aggregation to thrombin persisted, validating the claim that thrombin induces aggregation by a third pathway unrelated to ADP and to thromboxane A2. Aggregation by collagen was markedly reduced by exposure of the platelets to PAF-acether or to aspirin; when both procedures were associated, aggregation was suppressed. Failure to desensitize the rabbit platelets to PAF-acether upon exposure to high amounts of it indicates the absence of irreversible membrane changes due to PAF-acether, and allows its use as a depleting procedure for the dense body materials, which does not affect platelet membrane components as is the case for thrombin.

摘要

在将兔血小板暴露于1微摩尔血小板激活因子(PAF-乙醚)后,研究了凝血酶、胶原蛋白、蛇毒成分convulxin和血小板激活因子(PAF-乙醚)诱导的ATP聚集和分泌情况。该浓度比诱导完全聚集所需浓度高约6个数量级,是从血小板中去除大部分可释放ATP所必需的。在仅分泌极少量ATP的条件下,耗尽ATP的血小板对PAF-乙醚、凝血酶和convulxin发生聚集,这证实这些物质不需要释放致密体成分来触发聚集。此外,当PAF-乙醚暴露与阿司匹林使血小板环氧化酶失活同时发生时,对凝血酶的聚集持续存在,证实了凝血酶通过与ADP和血栓素A2无关的第三条途径诱导聚集的说法。血小板暴露于PAF-乙醚或阿司匹林后,胶原蛋白诱导的聚集明显减少;当两种处理同时进行时,聚集受到抑制。兔血小板暴露于大量PAF-乙醚后未能对其脱敏,这表明不存在因PAF-乙醚导致的不可逆膜变化,并允许将其用作致密体物质的耗尽程序,这与凝血酶不同,它不会影响血小板膜成分。

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