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Molecular characterization of 20 small supernumerary marker chromosome cases using array comparative genomic hybridization and fluorescence in situ hybridization

机译:利用阵列比较基因组杂交和荧光原位杂交技术鉴定20个小数量染色体标记病例的分子特征

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摘要

The variability of a small supernumerary marker chromosome (sSMC)-related phenotype is determined by the molecular component, the size, and shape of the marker chromosome. As fluorescence in situ hybridization has limitations regarding the resolution, efficiency, and accuracy. Recently, array comparative genomic hybridization (aCGH) was used for sSMC characterization. In this study, twenty cases with sSMCs were characterized by aCGH and FISH. Chromosomal origin of the marker chromosomes were successfully identified in seventeen of them. For the three cases with negative aCGH results, two of them were more likely due to that the sSMCs only contained centromere heterochromatin, whereas the reason for the remaining case with negative aCGH finding was uncertain. In order to establish a stronger genotype-phenotype correlation for clinical service in the future and avoid miss characterization, more sSMC cases were needed to be detailed characterized. This will help to clarify the variable clinical characteristics of sSMCs and provide additional information to aid clinical service and future research.
机译:小的数字标记染色体(sSMC)相关表型的变异性由标记染色体的分子组成,大小和形状决定。由于荧光原位杂交在分辨率,效率和准确性方面具有局限性。最近,阵列比较基因组杂交(aCGH)用于sSMC表征。在这项研究中,以aCGH和FISH为特征的20例sSMC病例。在其中的17个中成功鉴定出标记染色体的染色体起源。对于3例aCGH结果阴性的病例,其中2例更有可能是因为sSMC仅包含着丝粒异染色质,而其余1例aCGH结果阴性的原因尚不确定。为了在将来为临床服务建立更强的基因型-表型相关性并避免遗漏特征,需要对更多的sSMC病例进行详细特征分析。这将有助于阐明sSMC的可变临床特征,并提供更多信息以帮助临床服务和未来研究。

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