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Profiles of Extracellular miRNA in Cerebrospinal Fluid and Serum from Patients with Alzheimers and Parkinsons Diseases Correlate with Disease Status and Features of Pathology

机译:阿尔茨海默氏病和帕金森氏病患者脑脊液和血清中细胞外miRNA的分布与疾病状况和病理特征相关

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摘要

The discovery and reliable detection of markers for neurodegenerative diseases have been complicated by the inaccessibility of the diseased tissue- such as the inability to biopsy or test tissue from the central nervous system directly. RNAs originating from hard to access tissues, such as neurons within the brain and spinal cord, have the potential to get to the periphery where they can be detected non-invasively. The formation and extracellular release of microvesicles and RNA binding proteins have been found to carry RNA from cells of the central nervous system to the periphery and protect the RNA from degradation. Extracellular miRNAs detectable in peripheral circulation can provide information about cellular changes associated with human health and disease. In order to associate miRNA signals present in cell-free peripheral biofluids with neurodegenerative disease status of patients with Alzheimer's and Parkinson's diseases, we assessed the miRNA content in cerebrospinal fluid and serum from postmortem subjects with full neuropathology evaluations. We profiled the miRNA content from 69 patients with Alzheimer's disease, 67 with Parkinson's disease and 78 neurologically normal controls using next generation small RNA sequencing (NGS). We report the average abundance of each detected miRNA in cerebrospinal fluid and in serum and describe 13 novel miRNAs that were identified. We correlated changes in miRNA expression with aspects of disease severity such as Braak stage, dementia status, plaque and tangle densities, and the presence and severity of Lewy body pathology. Many of the differentially expressed miRNAs detected in peripheral cell-free cerebrospinal fluid and serum were previously reported in the literature to be deregulated in brain tissue from patients with neurodegenerative disease. These data indicate that extracellular miRNAs detectable in the cerebrospinal fluid and serum are reflective of cell-based changes in pathology and can be used to assess disease progression and therapeutic efficacy.
机译:神经退行性疾病的标记物的发现和可靠检测由于患病组织的难以接近而变得复杂,例如无法直接从中枢神经系统进行活检或测试组织。来自难以进入的组织(例如大脑和脊髓内的神经元)的RNA可能到达周围区域,可以无创地检测到它们。已经发现微囊泡和RNA结合蛋白的形成和细胞外释放将RNA从中枢神经系统的细胞携带到外周并保护RNA免于降解。在外周循环中可检测到的细胞外miRNA可提供有关与人类健康和疾病相关的细胞变化的信息。为了将无细胞外周生物流体中存在的miRNA信号与阿尔茨海默氏病和帕金森氏病患者的神经退行性疾病状态相关联,我们通过全面的神经病理学评估评估了死后受试者脑脊液和血清中的miRNA含量。我们使用下一代小RNA测序(NGS)分析了69位阿尔茨海默氏病,67位帕金森氏病和78位神经系统正常对照患者的miRNA含量。我们报告脑脊髓液和血清中每个检测到的miRNA的平均丰度,并描述了已鉴定的13种新型miRNA。我们将miRNA表达的变化与疾病严重程度相关,例如Br​​aak分期,痴呆状态,斑块和缠结密度以及路易体病理的存在和严重程度。先前已有文献报道在外周无细胞性脑脊液和血清中检测到的许多差异表达的miRNA在神经退行性疾病患者的脑组织中被失调。这些数据表明,脑脊髓液和血清中可检测到的细胞外miRNA反映了病理中基于细胞的变化,可用于评估疾病进展和治疗效果。

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