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Hsp31 of Escherichia coli K-12 is glyoxalase III.

机译:大肠杆菌K-12的Hsp31是乙二醛酶III。

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摘要

Hsp31 encoded by hchA is known as a heat-inducible molecular chaperone. Although structure studies revealed that Hsp31 has a putative catalytic triad consisting of Asp-214, His-186 and Cys-185, its enzymatic function, besides weak amino-peptidase activity, is still unknown. We found that Hsp31 displays glyoxalase activity that catalyses the conversion of methylglyoxal (MG) to d-lactate without an additional cofactor. The glyoxalase activity was completely abolished in the hchA-deficient strain, confirming the relationship between the hchA gene and its enzymatic activity in vivo. Hsp31 exhibits Michaelis-Menten kinetics for substrates MG with K(m) and k(cat) of 1.43+/-0.12 mM and 156.9+/-5.5 min(1) respectively. The highest glyoxalase activity was found at 35-40 degrees C and pH of 6.0-8.0, and the activity was significantly inhibited by Cu(2), Fe(3) and Zn(2). Mutagenesis studies based on our evaluation of conserved catalytic residues revealed that the Cys-185 and Glu-77 were essential for catalysis, whereas His-186 was less crucial for enzymatic function, although it participates in the catalytic process. The stationary-phase Escherichia coli cells became more susceptible to MG when hchA was deleted, which was complemented by an expression of plasmid-encoded hchA. Furthermore, an accumulation of intracellular MG was observed in hchA-deficient strains.
机译:由hchA编码的Hsp31被称为热诱导分子伴侣。尽管结构研究表明Hsp31具有由Asp-214,His-186和Cys-185组成的推定催化三联体,但其酶功能以及弱的氨基肽酶活性仍然未知。我们发现Hsp31显示乙二醛酶活性,可催化甲基乙二醛(MG)转化为d-乳酸,而无需其他辅助因子。在hchA缺陷型菌株中,乙二醛酶活性被完全消除,证实了hchA基因与其体内酶活性之间的关系。 Hsp31对底物MG表现出Michaelis-Menten动力学,底物MG的K(m)和k(cat)分别为1.43 +/- 0.12 mM和156.9 +/- 5.5 min(1)。发现最高的乙二醛酶活性在35-40摄氏度和pH值为6.0-8.0时,该活性被Cu(2),Fe(3)和Zn(2)显着抑制。根据我们对保守催化残基的评估进行的诱变研究表明,Cys-185和Glu-77对于催化必不可少,而His-186对酶的功能影响较小,尽管它参与了催化过程。缺失hchA后,固定相的大肠杆菌细胞对MG更加敏感,这可以通过质粒编码的hchA的表达来补充。此外,在hchA缺陷型菌株中观察到细胞内MG的积累。

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