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哺乳动物醛氧化酶基因家族。

The mammalian aldehyde oxidase gene family.

机构信息

Laboratory of Molecular Biology, Department of Biochemistry and Molecular Pharmacology, Istituto di Ricerche Farmacologiche Mario Negri, via La Masa 19, 20156 Milano, Italy.

出版信息

Hum Genomics. 2009 Dec;4(2):119-30. doi: 10.1186/1479-7364-4-2-119.

Abstract

Aldehyde oxidases (EC 1.2.3.1) are a small group of structurally conserved cytosolic proteins represented in both the animal and plant kingdoms. In vertebrates, aldehyde oxidases constitute the small sub-family of molybdo-flavoenzymes, along with the evolutionarily and structurally related protein, xanthine oxidoreductase. These enzymes require a molybdo-pterin cofactor (molybdenum cofactor, MoCo) and flavin adenine dinucleotide for their catalytic activity. Aldehyde oxidases have broad substrate specificity and catalyse the hydroxylation of N-heterocycles and the oxidation of aldehydes to the corresponding acid. In humans, a single aldehyde oxidase gene ( AOX1 ) and two pseudogenes clustering on a short stretch of chromosome 2q are known. In other mammals, a variable number of structurally conserved aldehyde oxidase genes has been described. Four genes ( Aox1 , Aox3 , Aox4 and Aox3l1 ), coding for an equivalent number of catalytically active enzymes, are present in the mouse and rat genomes. Although human AOX1 and its homologous proteins are best known as drug metabolising enzymes, the physiological substrate(s) and function(s) are as yet unknown. The present paper provides an update of the available information on the evolutionary history, tissue- and cell-specific distribution and function of mammalian aldehyde oxidases.

摘要

醛氧化酶(EC 1.2.3.1)是一个结构保守的细胞溶质蛋白小家族,存在于动物和植物界。在脊椎动物中,醛氧化酶与进化和结构相关的蛋白黄嘌呤氧化还原酶一起构成钼黄素酶的小亚家族。这些酶需要钼喋呤辅酶(钼辅酶,MoCo)和黄素腺嘌呤二核苷酸才能发挥其催化活性。醛氧化酶具有广泛的底物特异性,可催化 N-杂环的羟化和醛的氧化,生成相应的酸。在人类中,已知有一个单一的醛氧化酶基因(AOX1)和两个位于短臂 2q 上的假基因簇。在其他哺乳动物中,已经描述了数量可变的结构保守的醛氧化酶基因。在鼠和大鼠基因组中存在四个基因(Aox1、Aox3、Aox4 和 Aox3l1),编码数量相等的具有催化活性的酶。尽管人类 AOX1 及其同源蛋白作为药物代谢酶最为人所知,但它们的生理底物和功能仍未知。本文提供了有关哺乳动物醛氧化酶的进化历史、组织和细胞特异性分布和功能的最新信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e278/3525200/e41ecaf4e926/1479-7364-4-2-119-1.jpg

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