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稀释血浆的活化部分凝血活酶时间:因纤维蛋白检测方法导致的变异性。

The activated partial thromboplastin time of diluted plasma: variability due to the method of fibrin detection.

作者信息

Johnstone I B

出版信息

Can J Comp Med. 1984 Apr;48(2):198-201.

Abstract

The purpose of this study was to determine the effects of the dilution of plasma (1/3 in saline) on the kinetics of fibrin generation in the activated partial thromboplastin time (APTT) assay. The diluted APTT is considered to increase the sensitivity of the APTT test however, studies in our laboratory using an electro-optical fibrin detection system failed to show significant differences in APTT values obtained with diluted and undiluted canine plasma. Seventeen plasmas, including plasmas moderately and markedly deficient in intrinsic factor activity were assayed in the undiluted and diluted APTT assay using two methods for fibrin endpoint detection; a visual "tilt-tube" technique and an electro-optical detection system. In the former technique the endpoint was the formation of a visible fibrin web or clot; in the latter procedure the end point was the first detection of a change in optical density of the plasma. Optical density changes during fibrin formation were also recorded ( thrombokinetograms ). The results indicated that the electro-optical fibrin detection system failed to identify a prolongation of the APTT as a result of 1/3 plasma dilution; a prolongation that was consistently observed with the visual fibrin detection technique. Plasma dilution however, did significantly reduce the rate of fibrin production as indicated by the thrombokinetogram profile. It was concluded that the dilution of plasma with saline, as has been used to increase the sensitivity of the APTT assay procedure, has little effect on the time of onset of fibrin formation in a given plasma. The major effect appears to be on the way in which fibrin forms in that the polymerization/crosslinkage events associated with macroscopic fibrin production are delayed.

摘要

本研究的目的是确定在活化部分凝血活酶时间(APTT)测定中血浆稀释(用生理盐水稀释至1/3)对纤维蛋白生成动力学的影响。稀释后的APTT被认为可提高APTT试验的灵敏度,然而,我们实验室使用电光纤维蛋白检测系统的研究未能显示出用稀释和未稀释的犬血浆获得的APTT值有显著差异。使用两种纤维蛋白终点检测方法,对17份血浆进行了未稀释和稀释APTT测定,这些血浆包括中度和明显缺乏内源性因子活性的血浆;一种是视觉“倾斜管”技术,另一种是电光检测系统。在前一种技术中,终点是可见纤维蛋白网或凝块的形成;在后一种方法中,终点是首次检测到血浆光密度的变化。还记录了纤维蛋白形成过程中的光密度变化(血栓动图)。结果表明,电光纤维蛋白检测系统未能识别出由于血浆1/3稀释导致的APTT延长;而视觉纤维蛋白检测技术始终观察到这种延长。然而,血浆稀释确实显著降低了血栓动图所示的纤维蛋白生成速率。得出的结论是,如用于提高APTT测定程序灵敏度那样,用生理盐水稀释血浆对给定血浆中纤维蛋白形成的起始时间影响很小。主要影响似乎在于纤维蛋白形成的方式,即与宏观纤维蛋白产生相关的聚合/交联事件被延迟。

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