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Noninvasive characterization of Alzheimer’s disease by circulating, cell-free messenger RNA next-generation sequencing

机译:通过循环,无细胞信使RNA下一代测序进行阿尔茨海默病的非侵入性表征

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The lack of accessible noninvasive tools to examine the molecular alterations occurring in the brain limits our understanding of the causes and progression of Alzheimer’s disease (AD), as well as the identification of effective therapeutic strategies. Here, we conducted a comprehensive profiling of circulating, cell-free messenger RNA (cf-mRNA) in plasma of 126 patients with AD and 116 healthy controls of similar age. We identified 2591 dysregulated genes in the cf-mRNA of patients with AD, which are enriched in biological processes well known to be associated with AD. Dysregulated genes included brain-specific genes and resembled those identified to be dysregulated in postmortem AD brain tissue. Furthermore, we identified disease-relevant circulating gene transcripts that correlated with the severity of cognitive impairment. These data highlight the potential of high-throughput cf-mRNA sequencing to evaluate AD-related pathophysiological alterations in the brain, leading to precision healthcare solutions that could improve AD patient management.
机译:缺乏无障碍的非侵入性工具来检查大脑中发生的分子改变限制了我们对阿尔茨海默病(AD)的原因和进展的理解,以及鉴定有效的治疗策略。在这里,我们在126名患者的血浆中进行了循环,无细胞信使RNA(CF-mRNA)的全面分析,并进行了同类年龄的116例健康控制。我们在AD的患者的CF-mRNA中鉴定了2591个失调基因,其富含生物过程富人,该方法已知与AD相关。失调的基因包括脑特异性基因,并类似于鉴定的那些鉴定在淘汰后的AD脑组织中具有失调的基因。此外,我们鉴定了与认知障碍严重程度相关的疾病相关的循环基因转录物。这些数据突出了高通量CF-mRNA测序的潜力,以评估大脑中的广泛病理生理改变,导致精确的医疗保健解决方案,可以改善AD患者管理。

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