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鼠伤寒沙门氏菌cbiK在钴胺素(维生素B12)和siroheme生物合成中的作用。

A role for Salmonella typhimurium cbiK in cobalamin (vitamin B12) and siroheme biosynthesis.

作者信息

Raux E, Thermes C, Heathcote P, Rambach A, Warren M J

机构信息

Department of Molecular Genetics, Institute of Ophthalmology, University College London, United Kingdom.

出版信息

J Bacteriol. 1997 May;179(10):3202-12. doi: 10.1128/jb.179.10.3202-3212.1997.

Abstract

The role of cbiK, a gene found encoded within the Salmonella typhimurium cob operon, has been investigated by studying its in vivo function in Escherichia coli. First, it was found that cbiK is not required for cobalamin biosynthesis in the presence of a genomic cysG gene (encoding siroheme synthase) background. Second, in the absence of a genomic cysG gene, cobalamin biosynthesis in E. coli was found to be dependent upon the presence of cobA(P. denitrificans) (encoding the uroporphyrinogen III methyltransferase from Pseudomonas denitrificans) and cbiK. Third, complementation of the cysteine auxotrophy of the E. coli cysG deletion strain 302delta a could be attained by the combined presence of cobA(P. denitrificans) and the S. typhimurium cbiK gene. Collectively these results suggest that CbiK can function in fashion analogous to that of the N-terminal domain of CysG (CysG(B)), which catalyzes the final two steps in siroheme synthesis, i.e., NAD-dependent dehydrogenation of precorrin-2 to sirohydrochlorin and ferrochelation. Thus, phenotypically CysG(B) and CbiK have very similar properties in vivo, although the two proteins do not have any sequence similarity. In comparison to CysG, CbiK appears to have a greater affinity for Co2+ than for Fe2+, and it is likely that cbiK encodes an enzyme whose primary role is that of a cobalt chelatase in corrin biosynthesis.

摘要

cbiK是在鼠伤寒沙门氏菌钴胺素操纵子中发现的一个编码基因,通过研究其在大肠杆菌中的体内功能对其作用进行了调查。首先,发现在存在基因组cysG基因(编码 siro 血红素合酶)的背景下,钴胺素生物合成不需要cbiK。其次,在没有基因组cysG基因的情况下,发现大肠杆菌中的钴胺素生物合成依赖于cobA(反硝化假单胞菌)(编码来自反硝化假单胞菌的尿卟啉原III甲基转移酶)和cbiK的存在。第三,大肠杆菌cysG缺失菌株302delta a的半胱氨酸营养缺陷型的互补可以通过cobA(反硝化假单胞菌)和鼠伤寒沙门氏菌cbiK基因的共同存在来实现。这些结果共同表明,CbiK的功能方式类似于CysG的N端结构域(CysG(B)),后者催化siro血红素合成的最后两步,即依赖NAD的预钴胺素-2脱氢生成 siro 氢氯化血红素和铁螯合。因此,尽管这两种蛋白质没有任何序列相似性,但在体内CysG(B)和CbiK在表型上具有非常相似的特性。与CysG相比,CbiK对Co2+的亲和力似乎比对Fe2+的亲和力更大,并且cbiK可能编码一种酶,其主要作用是在钴胺素生物合成中作为钴螯合酶。

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