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芳胺N-乙酰基转移酶——从药物代谢与药物遗传学到药理学干预新靶点的鉴定

Arylamine N-acetyltransferases--from drug metabolism and pharmacogenetics to identification of novel targets for pharmacological intervention.

作者信息

Sim Edith, Fakis Giannoulis, Laurieri Nicola, Boukouvala Sotiria

机构信息

Department of Pharmacology, University of Oxford, Mansfield Road, Oxford, United Kingdom.

出版信息

Adv Pharmacol. 2012;63:169-205. doi: 10.1016/B978-0-12-398339-8.00005-7.

DOI:10.1016/B978-0-12-398339-8.00005-7
PMID:22776642
Abstract

Arylamine N-acetyltransferases (NATs) are defined as xenobiotic metabolizing enzymes, adding an acetyl group from acetyl coenzyme A (CoA) to arylamines and arylhydrazines. NATs are found in organisms from bacteria and fungi to vertebrates. Several isoenzymes, often polymorphic, may be present in one organism. There are two functional polymorphic NATs in humans and polymorphisms in NAT2 underpinned pharmacogenetics as a discipline. NAT enzymes have had a role in important metabolic concepts: the identification of acetyl-CoA and endogenous metabolic roles in bacteria and in eukaryotic folate metabolism. In fungi, NAT is linked to formation of unique metabolites. A broad and exciting canvas of investigations has emerged over the past five years from fundamental studies on NAT enzymes. The role of human NAT1 in breast cancer where it is a biomarker and possible therapeutic target may also underlie NAT's early appearance during mammalian fetal development. Studies of NAT in Mycobacterium tuberculosis have identified potential therapeutic targets for tuberculosis whilst the role of NATs in fungi opens up potential toxicological intervention in agriculture. These developments are possible through the combination of genomics, enzymology and structural data. Strong binding of CoA to Bacillis anthracis NAT may point to divergent roles of NATs amongst organisms as does differential control of mammalian NAT gene expression. The powerful combination of phenotypic investigation following genetic manipulation of NAT genes from mice to mycobacteria has been coupled with generation of isoenzyme-specific inhibitors. This battery of molecular and systems biology approaches heralds a new era for NAT research in pharmacology and toxicology.

摘要

芳胺N - 乙酰基转移酶(NATs)被定义为外源性物质代谢酶,它将乙酰辅酶A(CoA)中的乙酰基添加到芳胺和芳基肼上。从细菌、真菌到脊椎动物的生物体中都能发现NATs。一种生物体中可能存在几种同工酶,且通常具有多态性。人类有两种功能性多态性NATs,NAT2中的多态性奠定了药物遗传学这门学科的基础。NAT酶在重要的代谢概念中发挥了作用:在细菌中乙酰辅酶A的鉴定以及在真核生物叶酸代谢中的内源性代谢作用。在真菌中,NAT与独特代谢产物的形成有关。在过去五年中,基于对NAT酶的基础研究,涌现出了广泛而令人兴奋的研究领域。人类NAT1在乳腺癌中作为生物标志物和可能的治疗靶点的作用,也可能是其在哺乳动物胎儿发育早期出现的原因。对结核分枝杆菌中NAT的研究确定了结核病的潜在治疗靶点,而NATs在真菌中的作用为农业领域的潜在毒理学干预开辟了道路。通过基因组学、酶学和结构数据的结合,这些进展成为可能。辅酶A与炭疽芽孢杆菌NAT的强结合可能表明NATs在不同生物体中的作用存在差异,哺乳动物NAT基因表达的差异调控也是如此。从对小鼠到分枝杆菌的NAT基因进行遗传操作后的表型研究,与同工酶特异性抑制剂的产生相结合,这种强大的组合预示着NAT在药理学和毒理学研究中的新时代。

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