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临床前安全性生物标志物前沿:微小RNA与信使RNA

Frontiers in preclinical safety biomarkers: microRNAs and messenger RNAs.

作者信息

Mikaelian Igor, Scicchitano Marshall, Mendes Odete, Thomas Roberta A, Leroy Bruce E

机构信息

Hoffmann-La Roche, Inc., Nutley, NJ 07110, USA.

出版信息

Toxicol Pathol. 2013 Jan;41(1):18-31. doi: 10.1177/0192623312448939. Epub 2012 Jun 1.

Abstract

The measurement of plasma microRNAs (miRNAs) and messenger RNAs (mRNAs) is the most recent effort to identify novel biomarkers in preclinical safety. These genomic markers often display tissue-specific expression, may be released from the tissues into the plasma during toxic events, change early and with high magnitude in tissues and in the blood during specific organ toxicities, and can be measured using multiplex formats. Their validation as biomarkers has been challenged by the technical difficulties. In particular, the concentration of miRNAs in the plasma depends on contamination by miRNAs originating from blood cells and platelets, and the relative fraction of miRNAs in complexes with Argonaute 2, high-density lipoproteins, and in exosomes and microvesicles. In spite of these hurdles, considerable progress has recently been made in assessing the potential value of miRNAs in the clinic, especially in cancer patients and cardiovascular diseases. The future of miRNAs and mRNAs as biomarkers of disease and organ toxicity depends on our ability to characterize their kinetics and to establish robust collection and measurement methods. This review covers the basic biology of miRNAs and the published literature on the use of miRNAs and mRNAs as biomarkers of specific target organ toxicity.

摘要

血浆微小RNA(miRNA)和信使RNA(mRNA)的测量是临床前安全性研究中识别新型生物标志物的最新尝试。这些基因组标志物通常表现出组织特异性表达,在毒性事件期间可能从组织释放到血浆中,在特定器官毒性过程中,组织和血液中的含量会早期且大幅度地变化,并且可以使用多重检测方法进行测量。它们作为生物标志物的验证受到技术难题的挑战。特别是,血浆中miRNA的浓度取决于源自血细胞和血小板的miRNA的污染,以及与AGO2、高密度脂蛋白形成复合物的miRNA、外泌体和微泡中miRNA的相对比例。尽管存在这些障碍,但最近在评估miRNA在临床中的潜在价值方面取得了相当大的进展,尤其是在癌症患者和心血管疾病方面。miRNA和mRNA作为疾病和器官毒性生物标志物的未来取决于我们表征其动力学以及建立可靠的采集和测量方法的能力。本综述涵盖了miRNA的基本生物学以及关于使用miRNA和mRNA作为特定靶器官毒性生物标志物的已发表文献。

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