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阿尔茨海默病(AD)脑脊液(CSF)和细胞外液(ECF)中的微小RNA(miRNA)物种形成。

microRNA (miRNA) speciation in Alzheimer's disease (AD) cerebrospinal fluid (CSF) and extracellular fluid (ECF).

作者信息

Alexandrov Peter N, Dua Prerna, Hill James M, Bhattacharjee Surjyadipta, Zhao Yuhai, Lukiw Walter J

机构信息

Russian Academy of Medical Sciences Moscow 113152, Russia.

出版信息

Int J Biochem Mol Biol. 2012;3(4):365-73. Epub 2012 Dec 24.

Abstract

Human cerebrospinal fluid (CSF), produced by the choroid plexus and secreted into the brain ventricles and subarachnoid space, plays critical roles in intra-cerebral transport and the biophysical and immune protection of the brain. CSF composition provides valuable insight into soluble pathogenic bio-markers that may be diagnostic for brain disease. In these experiments we analyzed amyloid beta (Aβ) peptide and micro RNA (miRNA) abundance in CSF and in short post-mortem interval (PMI <2.1 hr) brain tissue-derived extracellular fluid (ECF) from Alzheimer's disease (AD) and age-matched control neocortex. There was a trend for decreased abundance of Aβ42 in the CSF and ECF in AD but it did not reach statistical significance (mean age 72 yr; N=12; p0.06, ANOVA). The most abundant nucleic acids in AD CSF and ECF were miRNAs, and their speciation and inducibility were studied further. Fluorescent miRNA-array-based analysis indicated significant increases in miRNA-9, miRNA-125b, miRNA-146a, miRNA-155 in AD CSF and ECF (N=12; p<0.01, ANOVA). Primary human neuronal-glial (HNG) cell co-cultures stressed with AD-derived ECF also displayed an up-regulation of these miRNAs, an effect that was quenched using the anti-NF-кB agents caffeic acid phenethyl ester (CAPE) or 1-fluoro-2-[2-(4-methoxy-phenyl)-ethenyl]-benzene (CAY10512). Increases in miRNAs were confirmed independently using a highly sensitive LED-Northern dot-blot assay. Several of these NF-кB-sensitive miRNAs are known to be up-regulated in AD brain, and associate with the progressive spreading of inflammatory neurodegeneration. The results indicate that miRNA-9, miRNA-125b, miRNA-146a and miRNA-155 are CSF- and ECF-abundant, NF-кB-sensitive pro-inflammatory miRNAs, and their enrichment in circulating CSF and ECF suggest that they may be involved in the modulation or proliferation of miRNA-triggered pathogenic signaling throughout the brain and central nervous system (CNS).

摘要

人类脑脊液(CSF)由脉络丛产生,分泌到脑室和蛛网膜下腔,在脑内物质运输以及大脑的生物物理和免疫保护中发挥关键作用。脑脊液成分能为可能用于脑部疾病诊断的可溶性致病生物标志物提供有价值的见解。在这些实验中,我们分析了阿尔茨海默病(AD)和年龄匹配的对照新皮质的脑脊液以及死后短时间间隔(PMI<2.1小时)脑组织衍生的细胞外液(ECF)中β淀粉样蛋白(Aβ)肽和微小RNA(miRNA)的丰度。AD患者脑脊液和ECF中Aβ42丰度有下降趋势,但未达到统计学意义(平均年龄约72岁;N = 12;p≈0.06,方差分析)。AD脑脊液和ECF中最丰富的核酸是miRNA,对其种类和诱导性进行了进一步研究。基于荧光miRNA阵列的分析表明,AD脑脊液和ECF中miRNA - 9、miRNA - 125b、miRNA - 146a、miRNA - 155显著增加(N = 12;p<0.01,方差分析)。用AD衍生的ECF应激的原代人神经胶质(HNG)细胞共培养物也显示出这些miRNA的上调,使用抗NF - κB剂咖啡酸苯乙酯(CAPE)或1 - 氟 - 2 - [2 -(4 - 甲氧基 - 苯基) - 乙烯基] - 苯(CAY10512)可消除这种效应。使用高度灵敏的LED - Northern斑点印迹法独立证实了miRNA的增加。已知这些对NF - κB敏感的miRNA中有几种在AD脑中上调,并与炎症性神经退行性变的进行性扩散相关。结果表明,miRNA - 9、miRNA - 125b、miRNA - 146a和miRNA - 155是脑脊液和ECF中丰富的、对NF - κB敏感的促炎miRNA,它们在循环脑脊液和ECF中的富集表明它们可能参与了整个大脑和中枢神经系统(CNS)中miRNA触发的致病信号的调节或增殖。

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