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PXR variants: the impact on drug metabolism and therapeutic responses

机译:PXR变体:对药物代谢和治疗反应的影响

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摘要

The pregnane X receptor (PXR) plays an important and diverse role in mediating xenobiotic induction of drug-metabolizing enzymes and transporters. Several protein isoforms of PXR exist, and they have differential transcriptional activity upon target genes; transcript variants 3 (PXR3) and 4 (PXR4) do not induce target gene expression, whereas transcript variants 1 (PXR1) and 2 (PXR2) respond to agonist by activating target gene expression. PXR protein variants also display differences in protein–protein interactions; PXR1 interacts with p53, whereas PXR3 does not. Furthermore, the transcript variants of PXR that encode these protein isoforms are differentially regulated by methylation and deletions in the respective promoters of the variants, and their expression differs in various human cancers and also in cancerous tissue compared to adjacent normal tissues. PXR1 and PXR4 mRNA are downregulated by methylation in cancerous tissue and have divergent effects on cellular proliferation when ectopically overexpressed. Additional detailed and comparative mechanistic studies are required to predict the effect of PXR transcript variant expression on carcinogenesis, therapeutic response, and the development of toxicity.
机译:孕烷X受体(PXR)在介导异种药物代谢酶和转运蛋白的诱导中起着重要而多样的作用。存在几种PXR的蛋白质同工型,它们对靶基因具有不同的转录活性。转录变体3(PXR3)和4(PXR4)不诱导靶基因表达,而转录变体1(PXR1)和2(PXR2)通过激活靶基因表达来响应激动剂。 PXR蛋白质变体在蛋白质间相互作用中也表现出差异。 PXR1与p53相互作用,而PXR3不与p53相互作用。此外,编码这些蛋白质同工型的PXR的转录物变体通过变体的各个启动子中的甲基化和缺失而受到差异调节,并且与相邻的正常组织相比,它们在各种人类癌症以及癌性组织中的表达也不同。 PXR1和PXR4 mRNA在癌组织中被甲基化下调,并在异位过表达时对细胞增殖产生不同的影响。需要其他详细和比较的机理研究来预测PXR转录变体表达对癌变,治疗反应和毒性发展的影响。

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