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三磷酸二腺苷(Ap3A)通过释放二磷酸腺苷介导人类血小板聚集。

Diadenosine triphosphate (Ap3A) mediates human platelet aggregation by liberation of ADP.

作者信息

Lüthje J, Ogilvie A

出版信息

Biochem Biophys Res Commun. 1984 Feb 14;118(3):704-9. doi: 10.1016/0006-291x(84)91451-7.

Abstract

Human platelets store considerable amounts of diadenosine 51,5111-P1, P3-triphosphate, which is released together with the homologue diadenosine tetraphosphate (Ap4A) upon thrombin-induced aggregation (Lüthje,J. & Ogilvie,A. (1983) Biochem. Biophys. Res. Commun. 115, 253-260). We now report that, when added to platelet-rich plasma at 10-20 micron, diadenosine triphosphate gradually induces aggregation. The addition of diadenosine tetraphosphate antagonizes this effect by rapidly disaggregating the platelets. When another physiological but structurally unrelated stimulus, i.e. PAF (Platelet activating factor) is introduced into the system, diadenosine triphosphate drastically enhances and prolongs the aggregatory effect of PAF. Again, Ap4A is antagonistic in this system. The mechanism of Ap3A-stimulation can be explained by the slow and continuous liberation of ADP from Ap3A by the action of a hydrolyzing enzyme which is present in human plasma. Our studies suggest that Ap3A may be physiologically important in providing a relatively long-lived stimulus that can modulate platelet aggregation.

摘要

人血小板储存有大量的5′,5″′-P1,P3-三磷酸二腺苷,在凝血酶诱导的聚集过程中,它与同系物四磷酸二腺苷(Ap4A)一起释放(吕特耶,J.和奥格尔维,A.(1983年)《生物化学与生物物理学研究通讯》115,253 - 260)。我们现在报告,当以10 - 20微米的浓度添加到富含血小板的血浆中时,三磷酸二腺苷会逐渐诱导聚集。添加四磷酸二腺苷会通过迅速使血小板解聚来拮抗这种作用。当将另一种生理但结构不相关的刺激物,即血小板活化因子(PAF)引入该系统时,三磷酸二腺苷会极大地增强并延长PAF的聚集作用。同样,Ap4A在该系统中具有拮抗作用。三磷酸二腺苷刺激的机制可以通过人血浆中存在的一种水解酶的作用,使三磷酸二腺苷缓慢且持续地释放出二磷酸腺苷来解释。我们的研究表明,三磷酸二腺苷在提供一种可调节血小板聚集的相对长效刺激方面可能具有生理重要性。

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