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血液的微观流变学与光传输。III. 红细胞聚集体形成的速度。

Microrheology and light transmission of blood. III. The velocity of red cell aggregate formation.

作者信息

Schmid-Schönbein H, Kline K A, Heinich L, Volger E, Fischer T

出版信息

Pflugers Arch. 1975;354(4):299-317. doi: 10.1007/BF00587849.

Abstract

The formation of primary (rouleaux) and secondary (rouleaux networks) RCA was studied by microcinematography (12 frames/sec) and photometry in a counterrotating "rheoscope" chamber. The blood was first subjected to rapid viscometric flow (460 sec-1, all RBC dispersed and aligned in flow) and then brought abruptly to full stop. In normal human blood, primary and secondary RCA occurred simultaneously, and were completed within 8 to 10 sec after stop. Blood from pregnant women at term, known for its pronounced red cell aggregation, shows a dissociation between the formation of short primary rouleaux (initiated even before full stop and completed 1-2 see thereafter) and secondary RCA completed 3-5 see after stop. RCA increases the light transmission of blood (measured by an increase in photovoltage V), the process and its first derivative (dV/dt equals I) can be recorded. After flow stop, there is an exponential decay of I(I equals t-I-o with e-lambda-t). The half time of this decay is recorded and correlated to the kinetics of red cell aggregate formation In human blood the half time of this process varies between 1.0 and 6.0 sec. In suspensions of human RBC in artificial plasmas, t-1/2 decreases with increasing concentration of fibrinogen and/or Dextran 250000, the second component appearing at concentrations above 500 mg-%. The method lend sitself for the quantification of RCA in small blood samples (20 mul).

摘要

通过显微电影摄影术(12帧/秒)和光度测量法,在反向旋转的“血流观测仪”腔室中研究了原发性(叠连)和继发性(叠连网络)红细胞聚集(RCA)的形成过程。血液首先经历快速粘度计流动(460秒-1,所有红细胞在流动中分散并排列),然后突然停止。在正常人血液中,原发性和继发性RCA同时发生,并在停止后8至10秒内完成。足月孕妇的血液以其明显的红细胞聚集而闻名,显示出短原发性叠连的形成(甚至在完全停止前就开始,并在其后1 - 2秒内完成)与停止后3 - 5秒完成的继发性RCA之间的分离。RCA增加了血液的光传输(通过光电压V的增加来测量),该过程及其一阶导数(dV/dt等于I)可以被记录。血流停止后,I呈指数衰减(I等于I - o乘以e的负λt次方)。记录该衰减的半衰期,并将其与红细胞聚集体形成的动力学相关联。在人体血液中,该过程的半衰期在1.0至6.0秒之间变化。在人工血浆中的人红细胞悬浮液中,t - 1/2随着纤维蛋白原和/或右旋糖酐250000浓度的增加而降低,第二种成分在浓度高于500mg-%时出现。该方法适用于对小血样(20微升)中的RCA进行定量。

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