首页> 美国卫生研究院文献>The Journal of Experimental Medicine >THE LYSIS IN RABBITS OF INTRAVASCULAR BLOOD CLOTS BY THE STREPTOCOCCAL FIBRINOLYTIC SYSTEM (STREPTOKINASE)
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THE LYSIS IN RABBITS OF INTRAVASCULAR BLOOD CLOTS BY THE STREPTOCOCCAL FIBRINOLYTIC SYSTEM (STREPTOKINASE)

机译:链球菌纤溶酶系统(链激酶)裂解血管内血块的兔子

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摘要

1. Based upon quantitative estimations of the factors that promote or retard the development and activity of the streptococcal fibrinolytic phenomenon, an active lytic system was developed within the circulating blood stream of rabbits following the intravenous infusion of streptokinase. During the infusion of adequate doses of SK, an active lytic system was observed to be present within 30 minutes following the beginning of the experiment and remained present for periods of time ranging from 1 to 20 hours depending primarily upon the concentration of SK and the duration of the infusion. Some of the biochemical changes accompanying the lytic system in vivo were: (a) a striking fall in the plasminogen; (b) a moderate fall in the serum inhibitor and the fibrinogen; and, (c) a rise in the acid-soluble nitrogen. These changes were usually self-terminating within 24 hours following the infusion of SK. In earlier studies similar trends were observed in the chest fluid of patients with hemothorax and empyema treated locally with streptokinase (22). 2. Intravascular clots, induced artificially by local applications of sodium morrhuate within the ear vein of the rabbits, were observed to liquefy and disappear in 23 of 25 rabbits during the intravenous infusion of SK into the opposite ear. The average quantity of SK necessary to effect an active lytic system was found to be about 40,000 units per kilo per hour. The clot in the ear vein was observed to be lysed completely in periods of time ranging from 3 to 7 hours after the infusion of SK was begun. Maintenance of an active lytic system for 3 to 4 additional hours was required to prevent re-formation of the clots at the original site. In 3 of 4 rabbits in which clots did reform, ACTH had been given to combat the toxic effects of the streptococcal concentrates. 3. The toxicity of the unusually large dose of the streptococcal concentrates, containing measured amounts of SK, along with other identifiable and unknown substances, was considerable, inasmuch as 8 animals eventually died. No evidence of pulmonary infarction was observed at autopsy. The administration of ACTH appeared to prevent a fatal outcome in at least 3 of the rabbits. Further studies of toxicity are in progress.
机译:1.根据对促进或延迟链球菌纤溶现象发展和活动的因素的定量估计,在链激酶的静脉内输注后,在兔循环血流中建立了一个活性裂解系统。在注入足够剂量的SK的过程中,观察到活性裂解系统在实验开始后的30分钟内存在,并在1至20小时的时间内保持存在,这主要取决于SK的浓度和持续时间输液。体内裂解系统伴随的一些生化变化是:(a)纤溶酶原的急剧下降; (b)血清抑制剂和纤维蛋白原适度下降; (c)酸溶氮的增加。这些变化通常在注入SK后24小时内自行终止。在较早的研究中,在局部经链激酶治疗的血胸和脓胸患者的胸水中观察到了类似的趋势(22)。 2.观察到通过在兔的耳静脉内局部施用莫来酸钠而人工诱导的血管内凝块,在25只兔中的23只中,在将SK静脉内注入对侧耳中时液化并消失。发现实现活性裂解系统所需的SK平均量约为每小时每公斤40,000个单位。开始注入SK后3至7小时,观察到耳静脉内的血块被完全溶解。为了防止血块在原始部位重新形成,需要将主动裂解系统再维持3-4小时。在四只凝结的兔子中,有三只接受了ACTH来对抗链球菌浓缩物的毒性作用。 3.异常大量的链球菌浓缩物(含有一定量的SK)以及其他可识别和未知的物质的毒性非常可观,最终导致8只动物死亡。尸检未观察到肺梗塞的迹象。服用ACTH似乎可以防止至少3只兔子的致命结局。毒性的进一步研究正在进行中。

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