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微小 RNA 对过敏性疾病基因调控网络改变的影响。

The impact of microRNAs on alterations of gene regulatory networks in allergic diseases.

机构信息

Laboratory for Epigenetics & Environment, Centre National de Recherche en Génomique Humaine, CEA-Institut de Biologie François Jacob, Evry, France.

出版信息

Adv Protein Chem Struct Biol. 2020;120:237-312. doi: 10.1016/bs.apcsb.2019.11.006. Epub 2020 Feb 12.

Abstract

Allergic diseases including asthma are worldwide on the rise and contribute significantly to health expenditures. Allergic diseases are prototypic diseases with a strong gene by environment interaction component and epigenetic mechanisms might mediate the effects of the environment on the disease phenotype. MicroRNAs, small non-coding RNAs (miRNAs), regulate gene expression post-transcriptionally. Functional single-stranded miRNAs are generated in multiple steps of enzymatic processing from their precursors and mature miRNAs are included into the RNA-induced silencing complex (RISC). They imperfectly base-pair with the 3'UTR region of targeted genes leading to translational repression or mRNA decay. The cellular context and microenvironment as well the isoform of the mRNA control the dynamics and complexity of the regulatory circuits induced by miRNAs that regulate cell fate decisions and function. MiR-21, miR-146a/b and miR-155 are among the best understood miRNAs of the immune system and implicated in different diseases including allergic diseases. MiRNAs are implicated in the induction of the allergy reinforcing the Th2 phenotype (miR-19a, miR-24, miR-27), while other miRNAs promote regulatory T cells associated with allergen tolerance or unresponsiveness. In the current chapter we describe in detail the biogenesis and regulatory function of miRNAs and summarize current knowledge on miRNAs in allergic diseases and allergy relevant cell fate decisions focusing mainly on immune cells. Furthermore, we evoke the principles of regulatory loops and feedback mechanisms involving miRNAs on examples with relevance for allergic diseases. Finally, we show the potential of miRNAs and exosomes containing miRNAs present in several biological fluids that can be exploited with non-invasive procedures for diagnostic and potentially therapeutic purposes.

摘要

过敏性疾病包括哮喘在全球范围内呈上升趋势,并对医疗支出造成重大影响。过敏性疾病是具有强烈基因与环境相互作用成分和表观遗传机制的典型疾病,这些机制可能介导环境对疾病表型的影响。微小 RNA(miRNA)是一类小的非编码 RNA,可在后转录水平上调节基因表达。成熟的 miRNA 是由前体经过多个酶切步骤加工而成,并包含在 RNA 诱导的沉默复合物(RISC)中。它们与靶基因的 3'UTR 区域不完全碱基配对,导致翻译抑制或 mRNA 降解。细胞内环境和微环境以及 mRNA 的异构体控制着由 miRNA 诱导的调控回路的动态和复杂性,这些调控回路调节细胞命运决定和功能。miR-21、miR-146a/b 和 miR-155 是免疫系统中研究最深入的 miRNA 之一,与包括过敏性疾病在内的多种疾病有关。miRNAs 参与了过敏反应的诱导,增强了 Th2 表型(miR-19a、miR-24、miR-27),而其他 miRNAs 则促进与过敏原耐受或无反应相关的调节性 T 细胞。在本章中,我们详细描述了 miRNA 的生物发生和调节功能,并总结了目前关于 miRNA 在过敏性疾病和与过敏相关的细胞命运决定中的知识,重点关注免疫细胞。此外,我们以与过敏性疾病相关的实例为例,阐述了涉及 miRNA 的调控回路和反馈机制的原理。最后,我们展示了存在于几种生物流体中的 miRNA 和包含 miRNA 的外泌体的潜力,这些可以通过非侵入性程序进行利用,用于诊断和潜在的治疗目的。

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