二酰胺对人血小板聚集、细胞骨架蛋白及花生四烯酸代谢的影响

Influence of diamide on aggregation, cytoskeletal proteins, and arachidonic acid metabolism in human platelets.

作者信息

Caruso D, Galli G, Till U, Spangenberg P, Lösche W, Paoletti R

出版信息

Thromb Res. 1984 Oct 1;36(1):9-16. doi: 10.1016/0049-3848(84)90371-2.

Abstract

Simultaneous addition of diamide (azodicarboxylic acid-bis-dimethylamide, DIA), a SH-oxidizing agent, and collagen causes a deaggregation of otherwise irreversibly aggregating platelets. Thromboxane B2 (TXB2) and 12-HE-TE formation is inhibited depending on the concentration ratio between collagen and DIA. Thus, at 0.25 mM DIA and 20 micrograms/ml collagen neither TXB2 nor 12-HETE were measurable, but a full scale reversible aggregation is induced. Deaggregation is further attained by adding DIA to collagen-induced aggregates at a time, when maximum amplitude has been achieved. Investigation of arachidonic acid (AA) metabolites under these conditions revealed no influence of DIA on AA metabolism. Therefore, AA metabolization seems to play a minor role in collagen-induced aggregation and DIA-induced deaggregation. Polymerization of certain cytoskeletal proteins of the platelets, after addition of DIA, parallels DIA-induced deaggregation. DIA inhibits endogenous AA release, probably by interaction with platelet plasma membrane. DIA seems to inhibit the release of the alpha-granula protein thrombospondin.

摘要

同时添加二酰胺（偶氮二甲酸双二甲酰胺，DIA），一种巯基氧化剂，和胶原蛋白会使原本不可逆聚集的血小板解聚。血栓素B2（TXB2）和12-羟基二十碳四烯酸（12-HETE）的形成会根据胶原蛋白和DIA之间的浓度比受到抑制。因此，在0.25 mM DIA和20微克/毫升胶原蛋白的条件下，TXB2和12-HETE均无法检测到，但会诱导出完全可逆的聚集。当达到最大振幅时，通过向胶原蛋白诱导的聚集体中添加DIA可进一步实现解聚。在这些条件下对花生四烯酸（AA）代谢物的研究表明，DIA对AA代谢没有影响。因此，AA代谢在胶原蛋白诱导的聚集和DIA诱导的解聚中似乎起次要作用。添加DIA后，血小板某些细胞骨架蛋白的聚合与DIA诱导的解聚平行。DIA可能通过与血小板质膜相互作用抑制内源性AA释放。DIA似乎抑制α-颗粒蛋白血小板反应蛋白的释放。