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The elusive nature and diagnostics of misfolded Aβ oligomers.

机译:错误折叠的Aβ低聚物的难以捉摸的性质和诊断。

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Amyloid-beta (Aβ) peptide oligomers are believed to be the causative agents of Alzheimer’s disease (AD). Though post-mortem examination shows that insoluble fibrils are deposited in the brains of AD patients in the form of intracellular (tangles) and extracellular (plaques) deposits, it has been observed that cognitive impairment is linked to synaptic dysfunction in the stages of the illness well before the appearance of these mature deposits. Increasing evidence suggests that the most toxic forms of Aβ are soluble low-oligomer ligands whose amounts better correlate with the extent of cognitive loss in patients than those of fibrillar insoluble forms. Therefore, these ligands hold the key to a better understanding of AD prompting the search for clearer correlations between their structure and toxicity. The importance of such correlations and their diagnostic value for the early diagnosis of AD is discussed here with a particular emphasis on the transient nature and structural plasticity of misfolded Aβ oligomers.
机译:淀粉样蛋白(Aβ)肽寡聚物被认为是阿尔茨海默氏病(AD)的病原体。虽然验尸显示不溶性原纤维以细胞内(缠结)和细胞外(斑块)沉积的形式沉积在AD患者的大脑中,但已观察到在疾病阶段认知障碍与突触功能障碍有关。这些成熟矿床出现之前。越来越多的证据表明,Aβ最具毒性的形式是可溶性低聚体配体,其含量与原纤维不溶性形式更好地与患者的认知丧失程度相关。因此,这些配体是更好地了解AD的关键,从而促使人们寻求其结构与毒性之间更清晰的相关性。本文讨论了这种相关性的重要性及其对AD早期诊断的诊断价值,并特别强调了错误折叠的Aβ低聚物的瞬时性质和结构可塑性。

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