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硫胺素和4-硫尿苷生物合成过程中共享的一种酶ThiI,可能是一种通过过硫化物中间体起作用的硫转移酶的证据。

Evidence that ThiI, an enzyme shared between thiamin and 4-thiouridine biosynthesis, may be a sulfurtransferase that proceeds through a persulfide intermediate.

作者信息

Palenchar P M, Buck C J, Cheng H, Larson T J, Mueller E G

机构信息

Department of Chemistry and Biochemistry, University of Delaware, Newark, Delaware 19716, USA.

出版信息

J Biol Chem. 2000 Mar 24;275(12):8283-6. doi: 10.1074/jbc.275.12.8283.

DOI:10.1074/jbc.275.12.8283
PMID:10722656
Abstract

ThiI is an enzyme common to the biosynthetic pathways leading to both thiamin and 4-thiouridine in tRNA. Comparison of the ThiI sequence with protein sequences in the data bases revealed that the Escherichia coli enzyme contains a C-terminal extension displaying sequence similarity to the sulfurtransferase rhodanese. Cys-456 of ThiI aligns with the active site cysteine residue of rhodanese that transiently forms a persulfide during catalysis. We investigated the functional importance of this sequence similarity and discovered that, like rhodanese, ThiI catalyzes the transfer of sulfur from thiosulfate to cyanide. Mutation of Cys-456 to alanine impairs this sulfurtransferase activity, and the C456A ThiI is incapable of supporting generation of 4-thiouridine in tRNA both in vitro and in vivo. We therefore conclude that Cys-456 of ThiI is critical for activity and propose that Cys-456 transiently forms a persulfide during catalysis. To accommodate this hypothesis, we propose a general mechanism for sulfur transfer in which the terminal sulfur of the persulfide first acts as a nucleophile and is then transferred as an equivalent of S(2-) rather than S(0).

摘要

硫胺素合成酶I是参与硫胺素和tRNA中4-硫尿苷生物合成途径的一种常见酶。将硫胺素合成酶I的序列与数据库中的蛋白质序列进行比较后发现,大肠杆菌的这种酶含有一个C端延伸区域,该区域的序列与硫转移酶硫氰酸酶具有相似性。硫胺素合成酶I的半胱氨酸-456与硫氰酸酶的活性位点半胱氨酸残基对齐,后者在催化过程中会短暂形成过硫化物。我们研究了这种序列相似性的功能重要性,发现硫胺素合成酶I与硫氰酸酶一样,能催化硫从硫代硫酸盐转移至氰化物。将半胱氨酸-456突变为丙氨酸会损害这种硫转移酶的活性,且C456A硫胺素合成酶I在体外和体内均无法支持tRNA中4-硫尿苷的生成。因此,我们得出结论,硫胺素合成酶I的半胱氨酸-456对其活性至关重要,并提出半胱氨酸-456在催化过程中会短暂形成过硫化物。为了支持这一假设,我们提出了一种硫转移的通用机制,即过硫化物的末端硫首先作为亲核试剂,然后以S(2-)而非S(0)的等价物形式转移。

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