Mouse models of aneuploidy to understand chromosome disorders

被引:0
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作者
Justin Tosh
Victor Tybulewicz
Elizabeth M. C. Fisher
机构
[1] The Francis Crick Institute,Department of Immunology and Inflammation
[2] Imperial College,Department of Neuromuscular Disease
[3] University College London,Queen Square Motor Neuron Disease Centre, Institute of Neurology
[4] University College London,undefined
来源
Mammalian Genome | 2022年 / 33卷
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摘要
An organism or cell carrying a number of chromosomes that is not a multiple of the haploid count is in a state of aneuploidy. This condition results in significant changes in the level of expression of genes that are gained or lost from the aneuploid chromosome(s) and most cases in humans are not compatible with life. However, a few aneuploidies can lead to live births, typically associated with deleterious phenotypes. We do not understand why phenotypes arise from aneuploid syndromes in humans. Animal models have the potential to provide great insight, but less than a handful of mouse models of aneuploidy have been made, and no ideal system exists in which to study the effects of aneuploidy per se versus those of raised gene dosage. Here, we give an overview of human aneuploid syndromes, the effects on physiology of having an altered number of chromosomes and we present the currently available mouse models of aneuploidy, focusing on models of trisomy 21 (which causes Down syndrome) because this is the most common, and therefore, the most studied autosomal aneuploidy. Finally, we discuss the potential role of carrying an extra chromosome on aneuploid phenotypes, independent of changes in gene dosage, and methods by which this could be investigated further.
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页码:157 / 168
页数:11
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