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Ontogenetic and Pathogenetic Views on Somatic Chromosomal Mosaicism

机译:体细胞染色体镶嵌的遗传学和病因学观点

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摘要

Intercellular karyotypic variability has been a focus of genetic research for more than 50 years. It has been repeatedly shown that chromosome heterogeneity manifesting as chromosomal mosaicism is associated with a variety of human diseases. Due to the ability of changing dynamically throughout the ontogeny, chromosomal mosaicism may mediate genome/chromosome instability and intercellular diversity in health and disease in a bottleneck fashion. However, the ubiquity of negligibly small populations of cells with abnormal karyotypes results in difficulties of the interpretation and detection, which may be nonetheless solved by post-genomic cytogenomic technologies. In the post-genomic era, it has become possible to uncover molecular and cellular pathways to genome/chromosome instability (chromosomal mosaicism or heterogeneity) using advanced whole-genome scanning technologies and bioinformatic tools. Furthermore, the opportunities to determine the effect of chromosomal abnormalities on the cellular phenotype seem to be useful for uncovering the intrinsic consequences of chromosomal mosaicism. Accordingly, a post-genomic review of chromosomal mosaicism in the ontogenetic and pathogenetic contexts appears to be required. Here, we review chromosomal mosaicism in its widest sense and discuss further directions of cyto(post)genomic research dedicated to chromosomal heterogeneity.
机译:50多年来,细胞间核型变异性一直是基因研究的重点。反复表明,表现为染色体镶嵌的染色体异质性与多种人类疾病有关。由于在整个个体发育过程中动态变化的能力,染色体镶嵌可能以瓶颈方式介导健康和疾病中的基因组/染色体不稳定和细胞间多样性。然而,具有异常核型的小细胞群的普遍存在导致解释和检测困难,但是仍可以通过后基因组细胞基因组技术解决。在后基因组时代,使用先进的全基因组扫描技术和生物信息学工具来发现导致基因组/染色体不稳定(染色体镶嵌或异质性)的分子和细胞途径已成为可能。此外,确定染色体异常对细胞表型的影响的机会似乎对于揭示染色体镶嵌症的内在后果很有用。因此,似乎需要在个体发生和致病背景下对染色体镶嵌进行基因组后审查。在这里,我们从最广泛的意义上回顾染色体镶嵌,并讨论致力于染色体异质性的细胞(后)基因组研究的进一步方向。

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