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- W2547565291 abstract "Down syndrome (DS), caused by human trisomy 21 (Ts21), can be considered as a prototypical model for understanding the effects of chromosomal aneuploidies in other diseases. Human chromosome 21 (Hsa21) is syntenically conserved with three regions in the mouse genome. A review of recent advances in genetic modeling and analysis of DS. Using Cre/loxP-mediated chromosome engineering, a substantial number of new mouse models of DS have recently been generated, which facilitates better understanding of disease mechanisms in DS. Based on evolutionary conservation, Ts21 can be modeled by engineered triplication of Hsa21 syntenic regions in mice. The validity of the models is supported by the exhibition of DS-related phenotypes. Although substantial progress has been made, it remains a challenge to unravel the relative importance of specific candidate genes and molecular mechanisms underlying the various clinical phenotypes. Further understanding of mechanisms based on data from mouse models, in parallel with human studies, may lead to novel therapies for clinical manifestations of Ts21 and insights to the roles of aneuploidies in other developmental disorders and cancers." @default.
- W2547565291 created "2016-11-11" @default.
- W2547565291 creator A5009879178 @default.
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- W2547565291 creator A5058196168 @default.
- W2547565291 creator A5067025277 @default.
- W2547565291 creator A5091303921 @default.
- W2547565291 date "2016-10-27" @default.
- W2547565291 modified "2023-10-18" @default.
- W2547565291 title "Mouse-based genetic modeling and analysis of Down syndrome" @default.
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