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多种抗聚集前列腺素对人动脉粥样硬化病变处血小板沉积的体内调节作用。

In vivo modulation of platelet deposition on human atherosclerotic lesions by various antiaggregatory prostaglandins.

作者信息

Fitscha P, Kaliman J, O'Grady J, Sinzinger H

机构信息

2nd Department of Internal Medicine, University of Vienna, Austria.

出版信息

Folia Haematol Int Mag Klin Morphol Blutforsch. 1988;115(4):443-6.

PMID:2465949
Abstract

The influence of intravenous infusions of various prostaglandins on in vivo platelet function was studied after labelling of autologous platelets with 100 mu ci 111 indium-oxinesulfate in patients with peripheral vascular disease stage II according to FONTAINE. PGI2 (5 ng/kg/min) provoked a significant decrease of platelet deposition and a prolongation in platelet half-life time (74 +/- 6 vs 68 +/- 5 hours). PGE1 (25 ng/kg/min) failed to influence platelet deposition, but prolonged significantly platelet half-life time (82 +/- 6 vs 76 +/- 8 hours). CG 4203 (25 ng/kg/min) decreased significantly platelet deposition and prolonged significantly platelet half-life time (73 +/- 10 vs 67 +/- 11 hours). Iloprost (1 and 2 ng/kg/min) reduced significantly platelet deposition without dose relation. Half-life time was increased significantly after therapy compared to placebo (1 ng: 76 +/- 7 vs 69 +/- 7; 2 ng: 73 +/- 9 vs 67 +/- 9 hours).

摘要

根据丰坦分类法,对II期周围血管疾病患者,在用100微居里111铟-氧肟酸硫酸盐标记自体血小板后,研究了静脉输注各种前列腺素对体内血小板功能的影响。前列环素(PGI2,5纳克/千克/分钟)可使血小板沉积显著减少,血小板半衰期延长(74±6小时对68±5小时)。前列腺素E1(PGE1,25纳克/千克/分钟)对血小板沉积无影响,但可使血小板半衰期显著延长(82±6小时对76±8小时)。CG 4203(25纳克/千克/分钟)可使血小板沉积显著减少,血小板半衰期显著延长(73±10小时对67±11小时)。伊洛前列素(1和2纳克/千克/分钟)可显著减少血小板沉积,且无剂量关系。与安慰剂相比,治疗后半衰期显著延长(1纳克:76±7小时对69±7小时;2纳克:73±9小时对67±9小时)。

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