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产前酒精暴露会使患有慢性坐骨神经病变的成年雌性大鼠的脊髓和循环免疫细胞环状RNA表达失调。

Prenatal alcohol exposure dysregulates spinal and circulating immune cell circular RNA expression in adult female rats with chronic sciatic neuropathy.

作者信息

Noor Shahani, Pritha Ariana N, Pasmay Andrea A, Sanchez Jacob E, Sanchez Joshua J, Fernandez-Oropeza Annette K, Sun Melody S, Dell'Orco Michela, Davies Suzy, Savage Daniel D, Mellios Nikolaos, Milligan Erin D

机构信息

Department of Neurosciences, School of Medicine, University of New Mexico, Albuquerque, NM, United States.

出版信息

Front Neurosci. 2023 Jun 9;17:1180308. doi: 10.3389/fnins.2023.1180308. eCollection 2023.

Abstract

Alcohol consumption during pregnancy is associated with Fetal Alcohol Spectrum Disorders (FASD) that results in a continuum of central nervous system (CNS) deficits. Emerging evidence from both preclinical and clinical studies indicate that the biological vulnerability to chronic CNS disease in FASD populations is driven by aberrant neuroimmune actions. Our prior studies suggest that, following minor nerve injury, prenatal alcohol exposure (PAE) is a risk factor for developing adult-onset chronic pathological touch sensitivity or allodynia. Allodynia in PAE rats occurs concurrently with heightened proinflammatory peripheral and spinal glial-immune activation. However, minor nerve-injured control rats remain non-allodynic, and corresponding proinflammatory factors are unaltered. A comprehensive molecular understanding of the mechanism(s) that underlie PAE-induced proinflammatory bias during adulthood remains elusive. Non-coding circular RNAs (circRNAs) are emerging as novel modulators of gene expression. Here, we hypothesized that PAE induces dysregulation of circRNAs that are linked to immune function under basal and nerve-injured conditions during adulthood. Utilizing a microarray platform, we carried out the first systematic profiling of circRNAs in adult PAE rats, prior to and after minor nerve injury. The results demonstrate a unique circRNA profile in adult PAE rats without injury; 18 circRNAs in blood and 32 spinal circRNAs were differentially regulated. Following minor nerve injury, more than 100 differentially regulated spinal circRNAs were observed in allodynic PAE rats. Bioinformatic analysis identified that the parental genes of these circRNAs are linked to the NF-κB complex, a central transcription factor for pain-relevant proinflammatory cytokines. Quantitative real-time PCR was employed to measure levels of selected circRNAs and linear mRNA isoforms. We have validated that was significantly downregulated in blood leukocytes in PAE rats, concurrent with downregulation of mRNA levels. Spinal levels were upregulated in PAE rats, regardless of nerve injury. Additionally, PAE downregulated levels of and , which are linked to immune regulation. These results demonstrate that PAE exerts long-lasting dysregulation of circRNA expression in blood leukocytes and the spinal cord. Moreover, the spinal circRNA expression profile following peripheral nerve injury is differentially modulated by PAE, potentially contributing to PAE-induced neuroimmune dysregulation.

摘要

孕期饮酒与胎儿酒精谱系障碍(FASD)相关,该障碍会导致一系列中枢神经系统(CNS)缺陷。临床前和临床研究的新证据表明,FASD人群对慢性CNS疾病的生物学易感性是由异常的神经免疫作用驱动的。我们之前的研究表明,在轻微神经损伤后,产前酒精暴露(PAE)是成年后发生慢性病理性触觉敏感性或异常性疼痛的一个危险因素。PAE大鼠的异常性疼痛与促炎外周和脊髓胶质免疫激活增强同时发生。然而,轻微神经损伤的对照大鼠仍无异常性疼痛,相应的促炎因子也未改变。对成年期PAE诱导的促炎偏向的潜在机制进行全面的分子理解仍然难以捉摸。非编码环状RNA(circRNA)正成为基因表达的新型调节因子。在此,我们假设PAE会导致成年期基础和神经损伤条件下与免疫功能相关的circRNA失调。利用微阵列平台,我们首次对成年PAE大鼠在轻微神经损伤前后的circRNA进行了系统分析。结果显示成年未受伤PAE大鼠有独特的circRNA谱;血液中有18种circRNA和32种脊髓circRNA受到差异调节。轻微神经损伤后,在异常性疼痛的PAE大鼠中观察到100多种差异调节的脊髓circRNA。生物信息学分析确定这些circRNA的亲本基因与NF-κB复合体相关,NF-κB是与疼痛相关的促炎细胞因子的中心转录因子。采用定量实时PCR来测量选定circRNA和线性mRNA异构体的水平。我们已经验证,PAE大鼠血液白细胞中的 显著下调,同时 mRNA水平也下调。无论神经损伤与否,PAE大鼠脊髓中的 水平上调。此外,PAE下调了与免疫调节相关的 和 的水平。这些结果表明,PAE对血液白细胞和脊髓中的circRNA表达产生长期失调作用。此外,外周神经损伤后脊髓circRNA表达谱受到PAE的差异调节,这可能导致PAE诱导的神经免疫失调。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/444d/10288115/6fac8f7b56fd/fnins-17-1180308-g001.jpg

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