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Molecular and Cytogenetic Evaluation of a Patient with Ring Chromosome 13 and Discordant Results

机译:环形染色体13患者的分子和细胞遗传学评价和结果不一致

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We describe the case of a male newborn with ring chromosome 13 found to have dysmorphic features, growth retardation, imperforate anus, and ambiguous genitalia. An initial karyotype showed 46, XY, r(13)(p13q34) in the 30 cells analyzed. SNP microarray from peripheral blood revealed not only an 8.14-Mb 13q33.2q34 deletion, but also a duplication of 87.49 Mb suggesting partial trisomy 13q that the patient did not appear to have clinically. Further cytogenetic characterization detected 3 distinct cell lines in the repeated peripheral blood sample: 46, XY, r(13)(p13q34)[89]/46, XY, r(13; 13)(p13q34)[7]/45, XY,-13[5] and 2 in cultured fibroblasts: 46, XY, r(13)(p13q34)[65]/45, XY,-13[35]. Repeated molecular studies on peripheral blood and fibroblasts, however, failed to document the initially seen partial trisomy 13q. We postulate that the presence of duplicated material may be evidence of the high burden of duplicate rings in peripheral blood at any given time, with the high rates of cell death caused by mitotically unstable double rings accounting for the repeated microarray results that failed to detect any duplications. We emphasize the correlation between both cytogenetic and molecular studies with thorough clinical assessment and suggest that given the high sensitivity of newer molecular cytogenetic techniques, careful interpretation of results is critical in the context of ring chromosomes. (C) 2014 S. Karger AG, Basel
机译:我们描述了一个具有13号环染色体的男性新生儿的情况,该染色体具有畸形特征,生长迟缓,肛门无孔和生殖器模棱两可。最初的核型在所分析的30个细胞中显示46,XY,r(13)(p13q34)。来自外周血的SNP芯片不仅显示出8.14-Mb 13q33.2q34缺失,而且重复出现87.49 Mb,这表明该患者似乎没有临床上的部分13q三体性。进一步的细胞遗传学表征在重复的外周血样本中检测到3种不同的细胞系:46,XY,r(13)(p13q34)[89] / 46,XY,r(13; 13)(p13q34)[7] / 45,XY ,成纤维细胞中的-13,[13] [5]和2:XY,r(13)(p13q34)[65] / 45,XY,[13] [35]。然而,对外周血和成纤维细胞的反复分子研究未能证明最初看到的部分三体性13q。我们推测重复材料的存在可能是在任何给定时间外周血中重复环的高负担的证据,有丝分裂不稳定的双环导致的高细胞死亡率解释了重复的微阵列结果未能检测到任何重复。我们通过全面的临床评估来强调细胞遗传学和分子研究之间的相关性,并建议鉴于新型分子细胞遗传学技术的高度敏感性,对结果的仔细解释对于环形染色体至关重要。 (C)2014 S.Karger AG,巴塞尔

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