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人丙酰辅酶A羧化酶和丙酮酸羧化酶生物素结合位点周围的序列同源性。

Sequence homology around the biotin-binding site of human propionyl-CoA carboxylase and pyruvate carboxylase.

作者信息

Lamhonwah A M, Quan F, Gravel R A

出版信息

Arch Biochem Biophys. 1987 May 1;254(2):631-6. doi: 10.1016/0003-9861(87)90146-9.

Abstract

Biotin-dependent carboxylases require covalently bound biotin for enzymatic activity. The biotin is attached through a lysine residue, which in a number of bacterial, avian, and mammalian carboxylases, is found within the conserved sequence Ala-Met-Lys-Met. We have determined the partial nucleotide sequence of cDNA clones for human propionyl-CoA carboxylase and pyruvate carboxylase. The predicted amino acid sequence of both these proteins contains the conserved tetrapeptide 35 residues from the carboxy terminus. In addition, both proteins contain the tripeptide, Pro-Met-Pro, 26 residues toward the amino terminus from the biotin attachment site. The overall amino acid homology through this region is 43%. Similar findings have been made for the biotin-containing polypeptides of transcarboxylase of Propionibacterium shermanii and acetyl-CoA carboxylase of Escherichia coli (W. L. Maloy, B. U. Bowien, G. K. Zwolinski, K. G. Kumar, and H. G. Wood (1979) J. Biol. Chem. 254, 11615-11622). The implications of this sequence conservation with regard to the function and evolution of biotin-dependent carboxylases is discussed. We propose that the 60 amino acids surrounding the biotin site are bounded by a proline "hinge" and the carboxy terminus has remained conserved as a result of constraints imposed by biotinylation of the enzyme.

摘要

生物素依赖性羧化酶需要共价结合的生物素才能发挥酶活性。生物素通过赖氨酸残基连接,在许多细菌、禽类和哺乳动物的羧化酶中,该赖氨酸残基位于保守序列丙氨酸-甲硫氨酸-赖氨酸-甲硫氨酸内。我们已经确定了人丙酰辅酶A羧化酶和丙酮酸羧化酶的cDNA克隆的部分核苷酸序列。这两种蛋白质的预测氨基酸序列在羧基末端35个残基处都含有保守的四肽。此外,这两种蛋白质在生物素连接位点向氨基末端26个残基处都含有三肽脯氨酸-甲硫氨酸-脯氨酸。该区域的整体氨基酸同源性为43%。对于谢氏丙酸杆菌转羧酶和大肠杆菌乙酰辅酶A羧化酶的含生物素多肽也有类似的发现(W. L. 马洛伊、B. U. 鲍伊恩、G. K. 兹沃林斯基、K. G. 库马尔和H. G. 伍德(1979年)《生物化学杂志》254,11615 - 11622)。本文讨论了这种序列保守性对生物素依赖性羧化酶功能和进化的影响。我们提出,生物素位点周围的60个氨基酸由一个脯氨酸“铰链”界定,并且由于酶生物素化所施加的限制,羧基末端一直保持保守。

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