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镍/钴通透酶(NiCoTs)对镍(2+)亲和转运的比较研究及重组大肠杆菌镍(2+)生物积累的潜力。

Comparative study on Ni(2+)-affinity transport of nickel/cobalt permeases (NiCoTs) and the potential of recombinant Escherichia coli for Ni(2+) bioaccumulation.

机构信息

College of Life Science, Shenzhen Key Laboratory of Microbial Genetic Engineering, Shenzhen University, Shenzhen 518060, PR China.

出版信息

Bioresour Technol. 2013 Feb;130:69-74. doi: 10.1016/j.biortech.2012.11.133. Epub 2012 Dec 8.

Abstract

Comparative evaluation on Ni(2+)-uptake of two nickel-affinity transmembrane proteins (NiCoTs) respectively from Helocobacter pylori (NixA) and Staphylococcus aureus (NisA) was performed. Expression of NiCoTs alone did not promote Ni(2+) uptake of the recombinant strains and made the growth susceptible to Ni(2+). However, recombinant strains expressing both NiCoTs and Metallothionein (MT) showed enhanced tolerance to Ni(2+) and Ni(2+) uptake. The maximum Ni(2+)-uptake capacity of recombinant strain N1c expressing NixA+MT reached 83.33mgg(-1), higher than 45.45mgg(-1) of recombinant strain N1d expressing NisA+MT. N1c exhibited more effective Ni(2+) accumulation than N1d in the presence of Na(+), Co(2+) and Cd(2+). NiCoTs promoted intracellular Ni(2+) uptake of the recombinant strains. Phosphate groups dominated Ni(2+) binding of wild type Escherichia coli, but carboxyl groups contributed more for N1c and N1d. The result suggested that NixA has a higher specificity in Ni(2+) binding than NisA, and both NiCoTs and MT are important for Ni(2+) bioaccumulation.

摘要

分别来自幽门螺杆菌(NixA)和金黄色葡萄球菌(NisA)的两种镍亲和跨膜蛋白(NiCoTs)的镍吸收能力进行了比较评估。单独表达 NiCoTs 不会促进重组菌株的镍吸收,反而使生长对镍敏感。然而,同时表达 NiCoTs 和金属硫蛋白(MT)的重组菌株表现出对镍的耐受性增强和镍吸收增强。表达 NixA+MT 的重组菌株 N1c 的最大镍吸收能力达到 83.33mgg(-1),高于表达 NisA+MT 的重组菌株 N1d 的 45.45mgg(-1)。在存在 Na(+)、Co(2+)和 Cd(2+)的情况下,N1c 比 N1d 更有效地积累镍。NiCoTs 促进了重组菌株的细胞内镍吸收。磷酸基团主导野生型大肠杆菌的镍结合,但羧基对 N1c 和 N1d 的贡献更大。结果表明,NixA 在镍结合方面比 NisA 具有更高的特异性,并且 NiCoTs 和 MT 对镍的生物积累都很重要。

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