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在人血浆中培养的A组链球菌临床分离株对纤溶酶(原)获取情况的分析

Analysis of plasmin(ogen) acquisition by clinical isolates of group A streptococci incubated in human plasma.

作者信息

Wang H, Lottenberg R, Boyle M D

机构信息

Department of Microbiology, Medical College of Ohio, Toledo 43699-0008.

出版信息

J Infect Dis. 1994 Jan;169(1):143-9. doi: 10.1093/infdis/169.1.143.

Abstract

Group A streptococci isolated from throat swabs or blood cultures were compared for the expression of plasmin(ogen) receptors. The majority of isolates bound 125I-labeled Lys-plasmin and 125I-labeled Lys-plasminogen while displaying minimal reactivity with 125I-labeled Glu-plasminogen. All streptococcal isolates could acquire surface enzymatic activity when incubated in human plasma but not if the plasma had been depleted of plasminogen. The ability to acquire surface enzymatic activity was limited by the quantity of streptokinase in the reaction mixture. There was no statistically significant difference between group A streptococci isolated from throat swabs and those from blood cultures with respect to their interaction with components of the fibrinolytic system in human plasma. However, these isolates could be divided into two groups based on their ability to acquire surface enzymatic activity when incubated in plasma with exogenous streptokinase. Surprisingly, the acquisition of surface enzymatic activity when incubated in plasma containing streptokinase was not always correlated with the plasmin(ogen) binding capacity determined by direct binding of radiolabeled ligands. Analysis of this phenomenon suggests that group A streptococci can use diverse mechanisms to acquire plasmin(ogen)-dependent enzymatic activity.

摘要

对从咽喉拭子或血培养物中分离出的A组链球菌进行纤溶酶(原)受体表达的比较。大多数分离株能结合125I标记的赖氨酸纤溶酶和125I标记的赖氨酸纤溶酶原,而与125I标记的谷氨酸纤溶酶原的反应性最小。所有链球菌分离株在人血浆中孵育时都能获得表面酶活性,但如果血浆中的纤溶酶原已耗尽则不能。获得表面酶活性的能力受反应混合物中链激酶量的限制。从咽喉拭子分离出的A组链球菌与从血培养物中分离出的A组链球菌在与人血浆中纤维蛋白溶解系统成分的相互作用方面,没有统计学上的显著差异。然而,根据这些分离株在含有外源性链激酶的血浆中孵育时获得表面酶活性的能力,可将它们分为两组。令人惊讶的是,在含有链激酶的血浆中孵育时获得表面酶活性并不总是与通过放射性标记配体的直接结合所确定的纤溶酶(原)结合能力相关。对这一现象的分析表明,A组链球菌可以利用多种机制来获得纤溶酶(原)依赖性酶活性。

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