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锯鳞蝰白腹亚种毒液中凝血因子IX/因子X结合蛋白的功能与序列特征

Functional and sequence characterization of coagulation factor IX/factor X-binding protein from the venom of Echis carinatus leucogaster.

作者信息

Chen Y L, Tsai I H

机构信息

Institute of Biological Chemistry, Academia Sinica, Taipei, Taiwan, Republic of China.

出版信息

Biochemistry. 1996 Apr 23;35(16):5264-71. doi: 10.1021/bi952520q.

Abstract

A new coagulation factor IX/factor X-binding protein (IX/X-bp) from Echis carinatus leucogaster venom has been purified and designated ECLV IX/X-bp. ECLV IX/X-bp binds factor IX and X in a Ca(2+)-dependent manner and is devoid of thrombin-inhibitory and platelet-aggregating activities. The apparent dissociation constants (Kd) for binding of ECLV IX/X-bp to factor IX and factor X are 6.6 and 125 nM, respectively. Upon the addition of Mg2+, the required Ca2+ concentration for optimal binding of ECLV IX/X-bp to factor IX and factor X was prominently reduced. Mg2+ also increases the affinity of factor X for the venom protein. Direct binding of IX/X-bp to factor IX and X could also be detected by far-Western blotting, and results of the experiment ruled out the lectin-like mechanism of ECLV IX/X-bp. The complete amino acid sequence and the disulfide pattern of ECLV IX/X-bp was deduced by enzymatic hydrolysis and automated sequencing of the S-pyridylethylated protein. The venom protein is a heterodimer with one subunit of 131 amino acid residues and another of 125 residues. Both subunits are homologous to each other and to other snake venom proteins of the C-type lectin superfamily.

摘要

一种来自锯鳞蝰白腹亚种毒液的新型凝血因子IX/因子X结合蛋白(IX/X-bp)已被纯化,并命名为ECLV IX/X-bp。ECLV IX/X-bp以Ca(2+)依赖的方式结合因子IX和X,且不具有凝血酶抑制活性和血小板聚集活性。ECLV IX/X-bp与因子IX和因子X结合的表观解离常数(Kd)分别为6.6和125 nM。加入Mg2+后,ECLV IX/X-bp与因子IX和因子X最佳结合所需的Ca2+浓度显著降低。Mg2+还增加了因子X对该毒液蛋白的亲和力。通过远缘Western印迹法也可检测到IX/X-bp与因子IX和X的直接结合,实验结果排除了ECLV IX/X-bp的凝集素样作用机制。通过对S-吡啶基乙基化蛋白进行酶解和自动测序,推导得到了ECLV IX/X-bp的完整氨基酸序列和二硫键模式。该毒液蛋白是一种异二聚体,一个亚基含有131个氨基酸残基,另一个亚基含有125个残基。两个亚基彼此同源,且与C型凝集素超家族的其他蛇毒蛋白同源。

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