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De Novo Small Supernumerary Marker Chromosomes Arising From Partial Trisomy Rescue

机译:<斜视> de novo 部分三元救援产生的小超值标记染色体

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Small supernumerary marker chromosomes (SMCs) are rare cytogenetic abnormalities. De novo small SMCs, particularly those combined with uniparental disomy (UPD), are assumed to result from incomplete trisomy rescue. Recently, a one-off cellular event designated as chromothripsis was reported as a mechanism for trisomy rescue in micronuclei. This Perspective article aims to highlight a possible association among trisomy rescue, chromothripsis, and SMCs. We propose that chromothripsis-mediated incomplete trisomy rescue in micronuclei underlies various chromosomal rearrangements including SMCs, although other mechanisms such as U-type exchange may also yield SMCs. These assumptions are primarily based on observations of previously reported patients with complex rearrangements and our patient with a small SMC. Given the high frequency of trisomic cells in human preimplantation embryos, chromothripsis-mediated trisomy rescue may be a physiologically important phenomenon. Nevertheless, trisomy rescue has a potential to produce UPD, SMCs, and other chromosomal rearrangements. The concepts of trisomy rescue, chromothripsis, and micronuclei provide novel insights into the mechanism for the maintenance and modification of human chromosomes.
机译:小超值标记染色体(SMC)是罕见的细胞遗传学异常。假设缺乏小型SMC,特别是那些与发单调性强性(UPD)相结合的小型SMC,这是由不完整的三重救援产生的。最近,称为Chromothripsis指定为Chromothripsis的一次性细胞事件作为微核的三胞质救援的机制。此透视文章旨在突出三元救援,Chromothripsis和SMC之间的可能性。我们提出染色体介导的分三术中的三胞质救援在微核下面是各种染色体重排,但其他机制如U型交换也可以产生SMC。这些假设主要基于先前报告的复杂重排患者和小型SMC患者的观察结果。鉴于人的预催化胚胎中三元素细胞的高频率,Chromothripsis介导的三胞质救援可能是生理学上的重要现象。尽管如此,三重奏救援有可能产生更新,SMC和其他染色体重排。三元救援,染色体和微核的概念为人类染色体维持和修饰的机制提供了新的洞察。

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