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miRNAs as Circulating Biomarkers for Alzheimer's Disease and Parkinson's Disease

机译:miRNAs作为阿尔茨海默氏病和帕金森氏病的循环生物标志物

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Detection of biomarkers for neurodegenerative disorders (NDDs) within brain tissues of Alzheimer's disease (AD) and Parkinson's disease (PD) patients has always been hampered by our inability to access and biopsy tissue of key brain regions implicated in disease occurrence and progression. Currently, diagnosis of NDDs is principally based on clinical observations of symptoms that present at later stages of disease progression, followed by neuroimaging and, possibly, CSF evaluation. One way to potentially detect and diagnose NDDs at a far earlier stage is to screen for abnormal levels of specific disease markers within the peripheral circulation of patients with NDDs. Increasing evidence suggests that there is dysregulation of microRNAs (miRNAs) in NDDs. Peripheral blood mononuclear cells, as well as biofluids, such as plasma, serum, urine and cerebrospinal fluid, contain miRNAs that can be identified and quantified. Circulating miRNAs within blood and other biofluids may thus be characterized and used as non-invasive, diagnostic biomarkers that facilitate the early detection of disease and potentially the continual monitoring of disease progression for NDDs such as AD and PD. Plainly, such a screen is only possible with a clear understanding of which miRNAs change with disease, and when these changes occur during the progression of AD and PD. Such information is becoming increasingly available and, in the near future, may not only support disease diagnosis, but provide the opportunity to evaluate therapeutic interventions earlier in the disease process.
机译:阿尔茨海默氏病(AD)和帕金森氏病(PD)患者脑组织中神经退行性疾病(NDD)生物标志物的检测一直受到我们无法进入和活检涉及疾病发生和发展的关键脑区域组织的阻碍。当前,对NDD的诊断主要是基于对疾病进展后期出现的症状的临床观察,然后进行神经影像学检查和可能的CSF评估。在较早阶段可能检测和诊断NDD的一种方法是在NDD患者外周循环中筛查特定疾病标志物的异常水平。越来越多的证据表明,NDD中存在microRNA(miRNA)失调。外周血单核细胞以及生物流体(例如血浆,血清,尿液和脑脊髓液)均含有可以识别和定量的miRNA。因此,血液和其他生物流体中的循环miRNA可以被表征并用作非侵入性诊断生物标记物,从而有助于疾病的早期检测,并可能持续监测NDD(例如AD和PD)的疾病进展。显然,只有明确了解哪些miRNA会随疾病而变化,以及何时在AD和PD进展期间发生这些变化,才可以进行此类筛选。这样的信息变得越来越可用,并且在不久的将来,不仅可以支持疾病诊断,而且可以提供在疾病过程早期评估治疗干预措施的机会。

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