期刊论文详细信息
Targeted deletion of the 9p21 non-coding coronary artery disease risk interval in mice
Article
关键词: CHROMOSOME 9P21;    MYOCARDIAL-INFARCTION;    TUMOR SUPPRESSION;    HEART-DISEASE;    INK4A LOCUS;    ASSOCIATION;    ATHEROSCLEROSIS;    EXPRESSION;    HYPERCHOLESTEROLEMIA;    SUSCEPTIBILITY;   
DOI  :  10.1038/nature08801
来源: SCIE
【 摘 要 】

Sequence polymorphisms in a 58-kilobase (kb) interval on chromosome 9p21 confer a markedly increased risk of coronary artery disease (CAD), the leading cause of death worldwide(1,2). The variants have a substantial effect on the epidemiology of CAD and other life-threatening vascular conditions because nearly one-quarter of Caucasians are homozygous for risk alleles. However, the risk interval is devoid of protein-coding genes and the mechanism linking the region to CAD risk has remained enigmatic. Here we show that deletion of the orthologous 70-kb non-coding interval on mouse chromosome 4 affects cardiac expression of neighbouring genes, as well as proliferation properties of vascular cells. Chr4(Delta 70kb/Delta 70kb) mice are viable, but show increased mortality both during development and as adults. Cardiac expression of two genes near the non-coding interval, Cdkn2a and Cdkn2b, is severely reduced in chr4(Delta 70kb/Delta 70kb) mice, indicating that distant-acting gene regulatory functions are located in the non-coding CAD risk interval. Allele-specific expression of Cdkn2b transcripts in heterozygous mice showed that the deletion affects expression through a cis-acting mechanism. Primary cultures of chr4(Delta 70kb/Delta 70kb) aortic smooth muscle cells exhibited excessive proliferation and diminished senescence, a cellular phenotype consistent with accelerated CAD pathogenesis. Taken together, our results provide direct evidence that the CAD risk interval has a pivotal role in regulation of cardiac Cdkn2a/b expression, and suggest that this region affects CAD progression by altering the dynamics of vascular cell proliferation.

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