Department of Obstetrics & Gynaecology, Li Ka Shing Institute of Health Sciences, The Chinese University of Hong Kong, Hong Kong, China.
BJOG. 2010 Mar;117(4):391-8. doi: 10.1111/j.1471-0528.2009.02470.x. Epub 2010 Jan 26.
Cytogenetic studies have demonstrated that duplications or deletions of entire chromosomes or microscopically visible aberrations are associated with specific congenital disorders. The subsequent development and application of microarray-based assays have established the importance of copy number variants (CNV) as a substantial source of genetic diversity in the human genome. Pathogenic CNVs are associated not only with birth defects and cancers, but also with neurodevelopmental disorders at birth or neurodegenerative diseases in adulthood. Unfortunately, the limited knowledge of the phenotypic effects of most CNVs has led to the classification of many CNVs as genomic imbalances of unknown clinical significance. This has caused many clinicians to resist the introduction of microarray technologies in detecting CNVs in a genome-wide manner for prenatal applications. This review summarises our current understanding of CNVs, the common detection methods, and the implications for human health and prenatal diagnosis.
细胞遗传学研究表明,整条染色体的重复或缺失或显微镜下可见的畸变与特定的先天性疾病有关。随后,基于微阵列的检测方法的发展和应用确立了拷贝数变异(CNV)作为人类基因组中遗传多样性的重要来源。致病性 CNV 不仅与出生缺陷和癌症有关,还与出生时的神经发育障碍或成年时的神经退行性疾病有关。不幸的是,由于对大多数 CNV 的表型效应的了解有限,许多 CNV 被归类为具有未知临床意义的基因组不平衡。这导致许多临床医生反对在产前应用中以全基因组的方式引入微阵列技术来检测 CNV。本综述总结了我们对 CNV 的现有认识,常见的检测方法,以及对人类健康和产前诊断的影响。
