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超声辐照下组织型纤溶酶原激活剂溶栓效果的评估:涉及测定血凝块中纤维蛋白降解产物的体外实验

Evaluation of the thrombolytic effect of tissue-type plasminogen activator with ultrasonic irradiation: in vitro experiment involving assay of the fibrin degradation products from the clot.

作者信息

Kimura M, Iijima S, Kobayashi K, Furuhata H

机构信息

Toxicology Laboratory, Kyoritsu College of Pharmacy, Tokyo, Japan.

出版信息

Biol Pharm Bull. 1994 Jan;17(1):126-30. doi: 10.1248/bpb.17.126.

Abstract

Previous studies show that the combined method using thrombolytic drugs and ultrasonic irradiation enhances the effect of thrombolysis in in vitro and in vivo experiments. However, the mechanism of the clot lysis was unclear. In previous studies the evaluation of the clot lysis effect was determined by the rate of decrease in clot weight or the decrease in radioisotope-labeled fibrinogen in the clot. However, it was unclear whether or not the fibrinogen in the clot was degraded. We measured quantitatively the fibrin degradation product, D-dimer (FDP-DD), produced from clots subjected to recombinant tissue-type plasminogen activator (rt-PA, 2.0 micrograms/ml), with and without ultrasonic irradiation. Two levels of continuous ultrasound were used, 300 kHz (100 V, 0.07 W/cm2) and 1 MHz (20 V, 0.4 W/cm2). The quantity of FDP-DD produced was 1.74 times at 300 kHz and 1.80 times at 1 MHz, greater than that measured in rt-PA solution without ultrasonic irradiation; clot lysis was not observed in normal saline with ultrasonic irradiation. Our experiment clarifies that the mechanism of clot lysis when subjected to a combination of drug and ultrasound leads to degradation of fibrin, allowing a quantitative measurement of the enhancement of clot lysis. A high correlation was observed between the FDP-DD produced from the clots and the rate of decrease in clot weight.

摘要

以往研究表明,在体外和体内实验中,使用溶栓药物与超声照射相结合的方法可增强溶栓效果。然而,血栓溶解的机制尚不清楚。在以往研究中,血栓溶解效果的评估是通过血栓重量的降低速率或血栓中放射性同位素标记纤维蛋白原的减少来确定的。然而,血栓中的纤维蛋白原是否降解并不明确。我们定量测量了在有和没有超声照射的情况下,重组组织型纤溶酶原激活剂(rt-PA,2.0微克/毫升)作用于血栓所产生的纤维蛋白降解产物D-二聚体(FDP-DD)。使用了两种连续超声水平,300千赫(100伏,0.07瓦/平方厘米)和1兆赫(20伏,0.4瓦/平方厘米)。在300千赫时产生的FDP-DD量是未进行超声照射的rt-PA溶液中测量值的1.74倍,在1兆赫时是1.80倍;在有超声照射的生理盐水中未观察到血栓溶解。我们的实验表明,药物与超声联合作用时血栓溶解的机制导致纤维蛋白降解,从而能够对血栓溶解增强情况进行定量测量。从血栓中产生的FDP-DD与血栓重量降低速率之间观察到高度相关性。

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