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从人抗凝血酶III三个二硫键的逐步还原推断其肝素结合结构域。一种分析部分还原蛋白质结构的有效方法。

Heparin binding domain of human antithrombin III inferred from the sequential reduction of its three disulfide linkages. An efficient method for structural analysis of partially reduced proteins.

作者信息

Sun X J, Chang J Y

机构信息

Pharmaceuticals Research Laboratories, Ciba-Geigy Ltd., Basel, Switzerland.

出版信息

J Biol Chem. 1989 Jul 5;264(19):11288-93.

PMID:2544589
Abstract

Human antithrombin III (AT-III) was partially reduced under mild conditions in the absence or presence of low molecular weight heparin. Quantitation of reduced disulfide bonds was facilitated by the application of a water-soluble color reagent, 4-N,N-dimethylaminoazobenzene-4'-iodoacetamido-2'-sulfonic acid (S-DABIA). The study shows that the three disulfide linkages of AT-III can be sequentially reduced, with Cys8-Cys128 being the most sensitive, followed by Cys21-Cys95, while Cys247-Cys430 is the most resistant to the mild reduction conditions. The rate of reduction of Cys8-Cys128 and Cys21-Cys95 was significantly decreased in the presence of heparin. The reduction of Cys8-Cys128 was also found to correlate quantitatively with the loss of heparin-accelerated antithrombin activity, heparin binding affinity, and heparin-induced fluorescence enhancement. These results suggest that Cys8-Cys128 is required for the integrity of the heparin binding domain of AT-III and support previous findings that lysyl residues surrounding Cys128 (Lys107, Lys114, Lys125, and Lys136) constitute an important part of the heparin binding site in AT-III.

摘要

在不存在或存在低分子量肝素的温和条件下,对人抗凝血酶III(AT-III)进行了部分还原。通过应用水溶性显色试剂4-N,N-二甲基氨基偶氮苯-4'-碘乙酰氨基-2'-磺酸(S-DABIA),便于对还原的二硫键进行定量分析。研究表明,AT-III的三个二硫键可以依次被还原,其中Cys8-Cys128最敏感,其次是Cys21-Cys95,而Cys247-Cys430对温和的还原条件最具抗性。在存在肝素的情况下,Cys8-Cys128和Cys21-Cys95的还原速率显著降低。还发现Cys8-Cys128的还原与肝素加速的抗凝血酶活性丧失、肝素结合亲和力以及肝素诱导的荧光增强在数量上相关。这些结果表明,Cys8-Cys128是AT-III肝素结合结构域完整性所必需的,并支持先前的研究结果,即Cys128周围的赖氨酸残基(Lys107、Lys114、Lys125和Lys136)构成了AT-III中肝素结合位点的重要部分。

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