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Aging and Intellectual Disability: Insights from Mouse Models of Down Syndrome

机译:衰老和智力残疾:唐氏综合症小鼠模型的见解

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摘要

Down syndrome (DS) is one of many causes of intellectual disability (ID), others including but not limited to, fetal alcohol syndrome. Fragile X syndrome, Rett syndrome, Williams syndrome, hypoxia, and infection. Down syndrome is characterized by a number of neurobiological problems resulting in learning and memory deficits and early onset Alzheimer's disease. The cognitive impairment in people with DS is virtually universal but varies considerably with respect to expressivity and severity. Significant advances in medical treatment and social inclusion have increased longevity in people with DS resulting in an increased aging population, thus highlighting the significance of early onset of dementia and the importance of identifying pharmacotherapies to treat DS-associated health complications in adults. Given its prevalence and established mouse models, this review will focus on ID in the DS population; specifically, the superimposed effect of aging on the complications already manifest in DS adults and the cognitive insights gained from studies on mouse models of DS.
机译:唐氏综合症(DS)是导致智障(ID)的众多原因之一,其他原因包括但不限于胎儿酒精综合症。易碎X综合征,Rett综合征,Williams综合征,缺氧和感染。唐氏综合症的特征是许多神经生物学问题,导致学习和记忆障碍以及阿尔茨海默氏病早发。 DS患者的认知障碍实际上是普遍的,但在表达力和严重性方面差异很大。药物治疗和社会包容性的重大进步已提高了DS患者的寿命,导致人口老龄化,从而凸显了痴呆症早发的重要性以及确定治疗成人DS相关健康并发症的药物治疗的重要性。鉴于其普遍性和已建立的小鼠模型,本文将重点关注DS人群中的ID。特别是,衰老对DS成人并发症的叠加作用已经显现,并且从对DS小鼠模型的研究中获得了认知见解。

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