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三羟甲基氨基甲烷对人和兔血小板对聚集剂反应的影响。

Effects of tris on responses of human and rabbit platelets to aggregating agents.

作者信息

Packham M A, Guccione M A, Nina M, Kinlough-Rathbone R L, Mustard J F

出版信息

Thromb Haemost. 1984 Apr 30;51(2):140-4.

PMID:6429880
Abstract

Despite reports that Tris [tris (hydroxymethyl)aminomethane] affects platelets, it is often used to buffer suspending media. Human or rabbit platelets were washed and resuspended in Tyrode solution containing apyrase and 0.35% albumin. Addition of 15 mM Tris partially inhibited primary aggregation induced by 10 microM ADP and inhibited aggregation and release of 14C-serotonin from prelabelled platelets stimulated with low concentrations of thrombin (0.05-0.2 U/mL), or collagen. Platelets resuspended in 15 mM Tris, 0.15 M NaCl, 0.35% albumin, pH 7.5, did not aggregate in response to 10 microM ADP whereas platelets in Tyrode-albumin aggregated extensively. Ca2+ (5 mM) did not overcome the inhibition of thrombin-induced aggregation. Tris (15 or 1.5 mM) potentiated aggregation and release induced by sodium arachidonate (20-50 microM) or the ionophore A23187 (0.6-1 microM). Pretreatment of platelets with aspirin did not prevent potentiation by A23187, indicating that it is not mediated through activation of the arachidonate pathway. The inhibitory and potentiating effects of Tris are similar to those of amino sugars, lysine, arginine and primary amines such as methylamine and cadaverine, and may represent general effects of amines on platelets. Potentiation of the effects of some aggregating agents and inhibition of others re-emphasizes the concept that there are several different mechanisms through which aggregation can occur. Tris-based buffers are unsuitable for platelet suspending media and their use as solvents for aggregating agents or inhibitors should be limited.

摘要

尽管有报道称三羟甲基氨基甲烷(Tris)会影响血小板,但它仍常被用于缓冲悬浮介质。将人或兔血小板洗涤后重悬于含有腺苷三磷酸双磷酸酶和0.35%白蛋白的Tyrode溶液中。加入15 mM Tris会部分抑制由10 μM ADP诱导的初级聚集,并抑制低浓度凝血酶(0.05 - 0.2 U/mL)或胶原蛋白刺激的预标记血小板中14C - 5 -羟色胺的聚集和释放。重悬于15 mM Tris、0.15 M NaCl、0.35%白蛋白、pH 7.5中的血小板,对10 μM ADP无反应而聚集,而在Tyrode -白蛋白中的血小板则大量聚集。Ca2 +(5 mM)不能克服对凝血酶诱导聚集的抑制作用。Tris(15 mM或1.5 mM)增强了花生四烯酸钠(20 - 50 μM)或离子载体A23187(0.6 - 1 μM)诱导的聚集和释放。用阿司匹林预处理血小板并不能阻止A23187的增强作用,表明其不是通过花生四烯酸途径的激活介导的。Tris的抑制和增强作用与氨基糖、赖氨酸、精氨酸以及甲胺和尸胺等伯胺的作用相似,可能代表了胺类对血小板的一般作用。某些聚集剂作用的增强和其他聚集剂作用的抑制再次强调了聚集可通过几种不同机制发生的概念。基于Tris的缓冲液不适用于血小板悬浮介质,其作为聚集剂或抑制剂溶剂的用途应受到限制。

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