首页> 外文期刊>American journal of medical genetics, Part A >A girl with neurofibromatosis type 1, atypical autism and mosaic ring chromosome 17.
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A girl with neurofibromatosis type 1, atypical autism and mosaic ring chromosome 17.

机译:一个患有1型神经纤维瘤病,非典型自闭症和镶嵌环染色体17的女孩。

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We describe a girl with neurofibromatosis type 1 (NF1), mild dysmorphic features, growth and mental retardation, autism, and mosaicism of ring chromosome 17 and chromosome 17 monosomy. The extent of genetic material deleted from the ring chromosome was determined using a combination of classical cytogenetics, fluorescence in situ hybridization (FISH) and multiplex ligation-dependent probe amplification (MLPA) to be 0.6-2.5 Mb on 17p, and up to about 10 Mb on 17q. Based on our observations and on a review of the literature we argue that in addition to a universal "ring syndrome" which is based on ring instability and is less specific for the chromosome involved, various ring chromosomes underlie their own characteristic phenotypes. We propose that the symptoms leading to the diagnosis of NF1 in our patient could be attributed to mosaic hemizygosity for the NF1 gene in some of her somatic cells. A similar mechanism or a direct involvement of respective disease genes in the aberration could possibly influence also the development of autism and other symptoms. We raise a question if the loss of one copy of chromosome 17 from a substantial fraction of somatic cells can have specific consequences also for future risks of the patient, for example, due to the mosaic hemizygosity for the BRCA1 and TP53 genes.
机译:我们描述了一个女孩,患有1型神经纤维瘤病(NF1),轻度畸形,成长和智力发育迟缓,自闭症以及环形17号染色​​体和17号染色​​体单体性的镶嵌症。使用经典细胞遗传学,荧光原位杂交(FISH)和多重连接依赖探针扩增(MLPA)的组合,确定从环形染色体上删除的遗传物质的程度在17p时为0.6-2.5 Mb,最高可达10p于17q播放Mb。根据我们的观察结果和对文献的评论,我们认为,除了一种普遍的“环综合征”是基于环的不稳定性,并且对所涉及的染色体的特异性较低之外,各种环染色体也构成了它们自己的特征表型。我们建议导致该患者诊断为NF1的症状可归因于她某些体细胞中NF1基因的镶嵌半合子性。各个疾病基因的类似机制或直接参与像差可能也可能影响自闭症和其他症状的发展。我们提出一个问题,即从相当大一部分的体细胞中丢失一个17号染色​​体拷贝是否还会对患者的未来风险产生特定的后果,例如,由于BRCA1和TP53基因的镶嵌半合子。

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