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凋亡调节因子在人类癌症中对miR-23a的表达:综述

Expression of miR-23a by apoptotic regulators in human cancer: A review.

作者信息

Roufayel Rabih, Kadry Seifedine

机构信息

a Department of Science , American University of the Middle East , Kuwait.

出版信息

Cancer Biol Ther. 2017 May 4;18(5):269-276. doi: 10.1080/15384047.2017.1310342. Epub 2017 Apr 28.

Abstract

MicroRNAs play fundamental roles in mammalian development, differentiation and cellular homeostasis by regulating essential processes such as proliferation, migration, metabolism, migration and cell death. These small non-coding RNAs are also responsible in RNA silencing, and in many developmental and pathological processes. Not surprisingly, miR-23a misexpression contributes to numerous diseases including cancer where certain miRNA genes have been classified as either oncogenes or tumor suppressor genes. Since a single microRNA is capable of targeting a large number of mRNA sequences, de-regulated miRNA expression has the ability to alter various transcripts and activate a wide range of cancer-related pathways. This review article documents reduced levels of mature miR-23a in various tumors, primarily due to epigenetic silencing or alterations in biogenesis pathways. Moreover, inhibition of miR-23a in stressed cells represent a general mechanism for inducing apoptosis and these microRNAs are showed to be regulated by molecular chaperon HSP70. Microarray expression analysis of miRNA overexpression or depletion is now used in the characterization of cancer development pathways and as a biomarker for early cancer detection.

摘要

微小RNA通过调控增殖、迁移、代谢、迁移和细胞死亡等基本过程,在哺乳动物发育、分化和细胞稳态中发挥着重要作用。这些小的非编码RNA还参与RNA沉默以及许多发育和病理过程。毫不奇怪,miR-23a的表达失调会导致包括癌症在内的多种疾病,其中某些miRNA基因已被归类为癌基因或肿瘤抑制基因。由于单个微小RNA能够靶向大量mRNA序列,因此miRNA表达失调能够改变各种转录本并激活多种癌症相关通路。这篇综述文章记录了各种肿瘤中成熟miR-23a水平的降低,主要是由于表观遗传沉默或生物合成途径的改变。此外,在应激细胞中抑制miR-23a是诱导细胞凋亡的一种普遍机制,并且这些微小RNA显示受分子伴侣HSP70调控。miRNA过表达或缺失的微阵列表达分析现在被用于癌症发展途径的表征以及作为早期癌症检测的生物标志物。

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