Gabbett M T, Peters G B, Carmichael J M, Darmanian A P, Collins F A
Genetic Health Queensland, Royal Children's Hospital, Brisbane, Queensland, Australia.
Clin Genet. 2008 Apr;73(4):353-9. doi: 10.1111/j.1399-0004.2007.00960.x. Epub 2008 Feb 13.
We report on a 4-year-old male with an interstitial tandem duplication of Xq21.1-q21.31 who presented with clinical features of Prader-Willi syndrome (PWS). The duplication was maternally inherited. Abnormalities of the X chromosome have previously been reported in association with a PWS phenotype, but to date, specific duplications of Xq21.1-q21.31 have not. We refined the chromosomal breakpoints seen on initial G-banded karyotyping in our case with comparative genomic hybridization by microarray (array CGH). The duplication was between 11.1 and 14.4 Mb in length and overlaps with three loci to which mental retardation with PWS-like features have been previously mapped, showing the utility of array CGH in helping to identify candidate genes. We conclude that duplication of chromosomal region Xq21.1-q21.31 potentially results in a PWS-like phenotype. Reviewing the literature on similar duplications, we further conclude that distal Xq duplications can result in features typically seen in infants with PWS, while proximal duplications can result in features typically seen in older children and adults with PWS. Duplications of chromosome Xq should be considered in the differential diagnosis of PWS, especially in males.
我们报告了一名4岁男性,其Xq21.1 - q21.31存在间质性串联重复,表现出普拉德 - 威利综合征(PWS)的临床特征。该重复是母系遗传的。先前曾报道X染色体异常与PWS表型相关,但迄今为止,Xq21.1 - q21.31的特定重复尚未见报道。我们通过微阵列比较基因组杂交(阵列CGH)对病例初始G带核型分析中所见的染色体断点进行了精细定位。该重复长度在11.1至14.4 Mb之间,与先前已定位到伴有PWS样特征智力发育迟缓的三个基因座重叠,显示了阵列CGH在帮助识别候选基因方面的效用。我们得出结论,染色体区域Xq21.1 - q21.31的重复可能导致PWS样表型。回顾关于类似重复的文献,我们进一步得出结论,Xq远端重复可导致PWS婴儿典型的特征,而近端重复可导致PWS大龄儿童和成人典型的特征。在PWS的鉴别诊断中应考虑Xq染色体重复,尤其是在男性中。
