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Molecular basis of pharmacotherapies for cognition in Down syndrome.

机译:唐氏综合症认知药物治疗的分子基础。

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Intellectual disability in Down syndrome (DS) ranges from low normal to severely impaired and has a significant impact on the quality-of-life of the individuals affected and their families. Because the incidence of DS remains at approximately 1 in 700 live births and the lifespan is now >50 years, development of pharmacotherapies for cognitive deficits is an important goal. DS is due to an extra copy of human chromosome 21 and has often been considered too complex a genetic abnormality to be amenable to intervention. However, recent successes in rescuing learning/memory impairments in a mouse model of DS suggest that this negative outlook may not be justified. In this contribution, we first review the DS phenotype, chromosome 21 gene content and mouse models. We then discuss recent successes and the remaining challenges in the identification of targets for and preclinical evaluation of potential therapeutics.
机译:唐氏综合症(DS)中的智力障碍从低正常到严重受损不等,并且对受影响个体及其家庭的生活质量产生重大影响。由于DS的发病率仍约为700例活产中的1例,并且寿命现已超过50岁,因此开发治疗认知功能障碍的药物疗法是一个重要目标。 DS是由于人类21号染色体的额外复制引起的,通常被认为是遗传异常过于复杂,难以进行干预。但是,最近在挽救DS小鼠模型中的学习/记忆障碍中取得的成功表明,这种消极的看法可能没有道理。在这项贡献中,我们首先回顾了DS表型,21号染色体基因含量和小鼠模型。然后,我们讨论了最近的成功以及潜在靶标的靶点识别和临床前评估中的剩余挑战。

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