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Arylamine N-acetyltransferase 1: A novel drug target in cancer development

机译:芳胺N-乙酰基转移酶1:癌症发展中的新型药物靶标

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The human arylamine N-acetyltransferases first attracted attention because of their role in drug metabolism. However, much of the current literature has focused on their role in the activation and detoxification of environmental carcinogens and how genetic polymorphisms in the genes create predispositions to increased or decreased cancer risk. There are two closely related genes on chromosome 8 that encode the two human arylamine N-acetyltransferases-NAT1 and NAT2. Although NAT2 has restricted tissue expression, NAT1 is found in almost all tissues of the body. There are several single-nucleotide polymorphisms in the protein coding and 3' -untranslated regions of the gene that affect enzyme activity. However, NAT1 is also regulated by post-translational and environmental factors, which may be of greater importance than genotype in determining tissue NAT1 activities. Recent studies have suggested a novel role for this enzyme in cancer cell growth. NAT1 is up-regulated in several cancer types, and overexpression can lead to increased survival and resistance to chemotherapy. Although a link to folate homeostasis has been suggested, many of the effects attributed to NAT1 and cancer cell growth remain to be explained. Nevertheless, the enzyme has emerged as a viable candidate for drug development, which should lead to small molecule inhibitors for preclinical and clinical evaluation.
机译:人芳基胺N-乙酰基转移酶由于其在药物代谢中的作用而首先引起关注。但是,当前的许多文献都集中在它们在环境致癌物的活化和解毒中的作用,以及基因中的遗传多态性如何导致增加或降低癌症风险的易感性。 8号染色体上有两个紧密相关的基因,它们编码两个人的芳基胺N-乙酰基转移酶-NAT1和NAT2。尽管NAT2限制了组织表达,但NAT1几乎存在于人体的所有组织中。在蛋白质的编码区和基因的3'-非翻译区中存在几种影响酶活性的单核苷酸多态性。但是,NAT1也受翻译后和环境因素的调节,这在确定组织NAT1活性方面可能比基因型更为重要。最近的研究表明该酶在癌细胞生长中具有新作用。 NAT1在几种癌症类型中均上调,过表达可导致存活率增加和对化学疗法的耐药性。尽管已经提出了与叶酸稳态的联系,但是许多归因于NAT1和癌细胞生长的作用仍有待解释。然而,该酶已成为药物开发的可行候选物,这应导致小分子抑制剂可用于临床前和临床评估。

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