From understanding to action: Exploring molecular connections of Down syndrome to Alzheimer's disease for targeted therapeutic approach

Sonal Sukreet, M. Rafii, R. Rissman
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Abstract

Abstract Down syndrome (DS) is caused by a third copy of chromosome 21. Alzheimer's disease (AD) is a neurodegenerative condition characterized by the deposition of amyloid‐beta (Aβ) plaques and neurofibrillary tangles in the brain. Both disorders have elevated Aβ, tau, dysregulated immune response, and inflammation. In people with DS, Hsa21 genes like APP and DYRK1A are overexpressed, causing an accumulation of amyloid and neurofibrillary tangles, and potentially contributing to an increased risk of AD. As a result, people with DS are a key demographic for research into AD therapeutics and prevention. The molecular links between DS and AD shed insights into the underlying causes of both diseases and highlight potential therapeutic targets. Also, using biomarkers for early diagnosis and treatment monitoring is an active area of research, and genetic screening for high‐risk individuals may enable earlier intervention. Finally, the fundamental mechanistic parallels between DS and AD emphasize the necessity for continued research into effective treatments and prevention measures for DS patients at risk for AD. Genetic screening with customized therapy approaches may help the DS population in current clinical studies and future biomarkers.
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从理解到行动:探索唐氏综合征与阿尔茨海默病之间的分子联系,寻找靶向治疗方法
摘要 唐氏综合征(DS)是由 21 号染色体的第三个拷贝引起的。阿尔茨海默病(AD)是一种神经退行性疾病,其特征是淀粉样β(Aβ)斑块和神经纤维缠结在大脑中沉积。这两种疾病都有 Aβ、tau 增高、免疫反应失调和炎症等症状。在 DS 患者中,APP 和 DYRK1A 等 Hsa21 基因过度表达,导致淀粉样蛋白和神经纤维缠结的积累,并有可能导致 AD 风险的增加。因此,DS患者是研究注意力缺失症治疗和预防的关键人群。DS和AD之间的分子联系揭示了这两种疾病的根本原因,并突出了潜在的治疗目标。此外,利用生物标志物进行早期诊断和治疗监测也是一个活跃的研究领域,而对高危人群进行基因筛查则可以实现早期干预。最后,DS 和 AD 在基本机理上的相似性强调了继续研究针对有 AD 风险的 DS 患者的有效治疗和预防措施的必要性。在当前的临床研究和未来的生物标志物研究中,基因筛查和定制治疗方法可能会对 DS 患者有所帮助。
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