Non-coding RNAs and neuroinflammation: implications for neurological disorders.

IF 2.8 4区医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL

Experimental Biology and Medicine Pub Date : 2024-02-28 eCollection Date: 2024-01-01 DOI:10.3389/ebm.2024.10120

Yvonne Chen, Julia Mateski, Linda Gerace, Jonathan Wheeler, Jan Burl, Bhavna Prakash, Cherie Svedin, Rebecca Amrick, Brian D Adams

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引用次数: 0

Abstract

Neuroinflammation is considered a balanced inflammatory response important in the intrinsic repair process after injury or infection. Under chronic states of disease, injury, or infection, persistent neuroinflammation results in a heightened presence of cytokines, chemokines, and reactive oxygen species that result in tissue damage. In the CNS, the surrounding microglia normally contain macrophages and other innate immune cells that perform active immune surveillance. The resulting cytokines produced by these macrophages affect the growth, development, and responsiveness of the microglia present in both white and gray matter regions of the CNS. Controlling the levels of these cytokines ultimately improves neurocognitive function and results in the repair of lesions associated with neurologic disease. MicroRNAs (miRNAs) are master regulators of the genome and subsequently control the activity of inflammatory responses crucial in sustaining a robust and acute immunological response towards an acute infection while dampening pathways that result in heightened levels of cytokines and chemokines associated with chronic neuroinflammation. Numerous reports have directly implicated miRNAs in controlling the abundance and activity of interleukins, TGF-B, NF-kB, and toll-like receptor-signaling intrinsically linked with the development of neurological disorders such as Parkinson's, ALS, epilepsy, Alzheimer's, and neuromuscular degeneration. This review is focused on discussing the role miRNAs play in regulating or initiating these chronic neurological states, many of which maintain the level and/or activity of neuron-specific secondary messengers. Dysregulated miRNAs present in the microglia, astrocytes, oligodendrocytes, and epididymal cells, contribute to an overall glial-specific inflammatory niche that impacts the activity of neuronal conductivity, signaling action potentials, neurotransmitter robustness, neuron-neuron specific communication, and neuron-muscular connections. Understanding which miRNAs regulate microglial activation is a crucial step forward in developing non-coding RNA-based therapeutics to treat and potentially correct the behavioral and cognitive deficits typically found in patients suffering from chronic neuroinflammation.

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非编码 RNA 与神经炎症：对神经系统疾病的影响。

神经炎症被认为是一种平衡的炎症反应，在损伤或感染后的内在修复过程中非常重要。在疾病、损伤或感染的慢性状态下，持续的神经炎症会导致细胞因子、趋化因子和活性氧的增加，从而造成组织损伤。在中枢神经系统中，周围的小胶质细胞通常含有巨噬细胞和其他先天性免疫细胞，它们会执行积极的免疫监视。这些巨噬细胞产生的细胞因子会影响中枢神经系统白质和灰质区域小胶质细胞的生长、发育和反应能力。控制这些细胞因子的水平最终会改善神经认知功能，并修复与神经系统疾病相关的病变。微小核糖核酸（miRNA）是基因组的主调控因子，随后控制炎症反应的活动，这对维持对急性感染的强大和急性免疫反应至关重要，同时抑制导致与慢性神经炎症相关的细胞因子和趋化因子水平升高的途径。许多报告都直接指出，miRNAs 控制着白细胞介素、TGF-B、NF-kB 和类收费受体信号的丰度和活性，而这些信号与帕金森氏症、渐冻人症、癫痫、阿尔茨海默氏症和神经肌肉变性等神经系统疾病的发展有着内在联系。这篇综述将重点讨论 miRNA 在调节或引发这些慢性神经系统疾病中的作用，其中许多疾病都会维持神经元特异性次级信使的水平和/或活性。存在于小胶质细胞、星形胶质细胞、少突胶质细胞和附睾细胞中的失调 miRNA 会导致胶质细胞特异性炎症生态位，从而影响神经元传导性、动作电位信号、神经递质稳健性、神经元-神经元特异性通信和神经元-肌肉连接的活动。了解哪些 miRNA 可调控小胶质细胞的活化是开发基于非编码 RNA 的疗法的关键一步，这种疗法可治疗并有可能纠正慢性神经炎症患者通常存在的行为和认知缺陷。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Experimental Biology and Medicine 医学-医学：研究与实验

CiteScore

6.00

自引率

0.00%

发文量

157

审稿时长

1 months

期刊介绍： Experimental Biology and Medicine (EBM) is a global, peer-reviewed journal dedicated to the publication of multidisciplinary and interdisciplinary research in the biomedical sciences. EBM provides both research and review articles as well as meeting symposia and brief communications. Articles in EBM represent cutting edge research at the overlapping junctions of the biological, physical and engineering sciences that impact upon the health and welfare of the world''s population. Topics covered in EBM include: Anatomy/Pathology; Biochemistry and Molecular Biology; Bioimaging; Biomedical Engineering; Bionanoscience; Cell and Developmental Biology; Endocrinology and Nutrition; Environmental Health/Biomarkers/Precision Medicine; Genomics, Proteomics, and Bioinformatics; Immunology/Microbiology/Virology; Mechanisms of Aging; Neuroscience; Pharmacology and Toxicology; Physiology; Stem Cell Biology; Structural Biology; Systems Biology and Microphysiological Systems; and Translational Research.