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首页> 外文期刊>Brain pathology >Brain‐derived and circulating vesicle profiles indicate neurovascular unit dysfunction in early Alzheimer’s disease
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Brain‐derived and circulating vesicle profiles indicate neurovascular unit dysfunction in early Alzheimer’s disease

机译:脑衍生的和循环囊泡谱表明早期阿尔茨海默病患者的神经血管单位功能障碍

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Abstract Vascular factors that reduce blood flow to the brain are involved in apparition and progression of dementia. We hypothesized that cerebral hypoperfusion (CH) might alter the molecular compositions of brain intercellular communication mechanisms while affecting the neurovascular unit in preclinical and clinical human dementias. To test that hypothesis, mice were subjected to bilateral common carotid stenosis (BCAS) and the molecular compositions of brain‐derived and circulating extracellular vesicles (EVs) were assessed. Murine brain vesicle profiles were then analyzed in parallel with brain EVs from post‐mortem subjects affected by preclinical Alzheimer’s Disease (AD) and mixed dementias. Brain EVs were identified with molecular mediators of hypoxia responses, neuroprotection and neurotoxicity in BCAS mice, patterns also partially resembled by subjects with preclinical AD and mixed dementias. Together these findings indicate that brain EVs represent a promising source of therapeutic targets and circulating markers of neurovascular insult in idiopathic dementias. Furthermore, the results obtained generate novel and compelling hypotheses about the molecular involvement of the vascular component in the etiology of human dementias.
机译:摘要减少血液流向大脑的血管因素参与痴呆症的幻影和进展。我们假设脑低渗(CH)可能改变脑细胞间通信机制的分子组成,同时影响临床前和临床人痴呆的神经血管单元。为了测试该假设,对小鼠进行双侧常见的颈动脉狭窄(BCA),评估脑衍生和循环细胞外囊泡(EVS)的分子组成。然后将鼠脑囊泡谱系与受验尸受试者的脑EV平行分析,受临床前阿尔茨海默病(AD)和混合痴呆影响。用BCAS小鼠的缺氧反应,神经保护和神经毒性的分子介质鉴定脑EVS,通过具有临床前AD和混合痴呆的受试者,也与受试者部分地相似的图案。这些结果表明,脑EVS代表了特发性痴呆中神经血管损伤的有前途的治疗目标和循环标志。此外,得到的结果产生了关于血管组分在人痴呆病因中的分子诱导的新颖和令人信服的假设。

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