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年龄相关的 miRNA 表达变化影响 GSTZ1 和其他药物代谢酶。

Age-Related Changes in miRNA Expression Influence GSTZ1 and Other Drug Metabolizing Enzymes.

机构信息

Departments of Medicinal Chemistry (S.C.J., C.J.W., M.O.J.), Pharmacotherapy and Translational Research (T.Y.L.), Medicine (P.W.S.), Biochemistry and Molecular Biology (P.W.S.), and Molecular Genetics and Microbiology (L.A.G., R.R.), University of Florida, Gainesville, Florida.

Departments of Medicinal Chemistry (S.C.J., C.J.W., M.O.J.), Pharmacotherapy and Translational Research (T.Y.L.), Medicine (P.W.S.), Biochemistry and Molecular Biology (P.W.S.), and Molecular Genetics and Microbiology (L.A.G., R.R.), University of Florida, Gainesville, Florida

出版信息

Drug Metab Dispos. 2020 Jul;48(7):563-569. doi: 10.1124/dmd.120.090639. Epub 2020 May 1.

Abstract

Previous work has shown that hepatic levels of human glutathione transferase zeta 1 (GSTZ1) protein, involved in tyrosine catabolism and responsible for metabolism of the investigational drug dichloroacetate, increase in cytosol after birth before reaching a plateau around age 7. However, the mechanism regulating this change of expression is still unknown, and previous studies showed that mRNA levels did not correlate with GSTZ1 protein expression. In this study, we addressed the hypothesis that microRNAs (miRNAs) could regulate expression of GSTZ1. We obtained liver samples from donors aged less than 1 year or older than 13 years and isolated total RNA for use in a microarray to identify miRNAs that were downregulated in the livers of adults compared with children. From a total of 2578 human miRNAs tested, 63 miRNAs were more than 2-fold down-regulated in adults, of which miR-376c-3p was predicted to bind to the 3' untranslated region of mRNA. There was an inverse correlation of miR-376c-3p and GSTZ1 protein expression in the liver samples. Using cell culture, we confirmed that miR-376c-3p could downregulate GSTZ1 protein expression. Our findings suggest that miR-376c-3p prevents production of GSTZ1 through inhibition of translation. These experiments further our understanding of GSTZ1 regulation. Furthermore, our array results provide a database resource for future studies on mechanisms regulating human hepatic developmental expression. SIGNIFICANCE STATEMENT: Hepatic glutathione transferase zeta 1 (GSTZ1) is responsible for metabolism of the tyrosine catabolite maleylacetoacetate as well as the investigational drug dichloroacetate. Through examination of microRNA (miRNA) expression in liver from infants and adults and studies in cells, we showed that expression of GSTZ1 is controlled by miRNA. This finding has application to the dosing regimen of the drug dichloroacetate. The miRNA expression profiles are provided and will prove useful for future studies of drug-metabolizing enzymes in infants and adults.

摘要

先前的工作表明,参与酪氨酸分解代谢并负责研究药物二氯乙酸代谢的人谷胱甘肽转移酶 ζ1(GSTZ1)蛋白在细胞质中的肝水平在出生后增加,然后在 7 岁左右达到稳定。然而,调节这种表达变化的机制尚不清楚,先前的研究表明,mRNA 水平与 GSTZ1 蛋白表达不相关。在这项研究中,我们提出了一个假设,即 microRNAs(miRNAs)可以调节 GSTZ1 的表达。我们从年龄小于 1 岁或大于 13 岁的供体中获得肝脏样本,并分离总 RNA,用于微阵列以鉴定与儿童相比在成人肝脏中下调的 miRNAs。在总共测试的 2578 个人类 miRNA 中,有 63 个 miRNA 在成人中下调超过 2 倍,其中 miR-376c-3p 被预测与 3'UTR 的结合。在肝样本中,miR-376c-3p 与 GSTZ1 蛋白表达呈负相关。通过细胞培养,我们证实 miR-376c-3p 可以下调 GSTZ1 蛋白表达。我们的研究结果表明,miR-376c-3p 通过抑制翻译来防止 GSTZ1 的产生。这些实验进一步加深了我们对 GSTZ1 调控的理解。此外,我们的阵列结果为未来研究调节人类肝脏发育表达的机制提供了数据库资源。意义声明:肝谷胱甘肽转移酶 ζ1(GSTZ1)负责代谢酪氨酸分解产物马来酰乙酰乙酸以及研究药物二氯乙酸。通过检查婴儿和成人肝脏中的 miRNA(miRNA)表达和细胞研究,我们表明 GSTZ1 的表达受 miRNA 控制。这一发现对二氯乙酸的给药方案有应用价值。提供了 miRNA 表达谱,将对未来研究婴儿和成人的药物代谢酶非常有用。

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本文引用的文献

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