包括SOX10在内的22q11.2q13重复会导致性反转、周围性脱髓鞘性神经病、中枢性髓鞘形成障碍性脑白质营养不良、瓦登伯革氏综合征和先天性巨结肠病。
22q11.2q13 duplication including SOX10 causes sex-reversal and peripheral demyelinating neuropathy, central dysmyelinating leukodystrophy, Waardenburg syndrome, and Hirschsprung disease.
作者信息
Falah Nadia, Posey Jennifer E, Thorson Willa, Benke Paul, Tekin Mustafa, Tarshish Brocha, Lupski James R, Harel Tamar
机构信息
Division of Clinical and Translational Genetics, Dr. John T. Macdonald Foundation Department of Human Genetics, John P. Hussman Institute for Human Genomics Miller School of Medicine, University of Miami and Jackson Memorial Hospital, Miami, Florida.
Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas.
出版信息
Am J Med Genet A. 2017 Apr;173(4):1066-1070. doi: 10.1002/ajmg.a.38109.
Abstract
Diagnosis of genetic syndromes may be difficult when specific components of a disorder manifest at a later age. We present a follow up of a previous report [Seeherunvong et al., (2004); AJMGA 127: 149-151], of an individual with 22q duplication and sex-reversal syndrome. The subject's phenotype evolved to include peripheral and central demyelination, Waardenburg syndrome type IV, and Hirschsprung disease (PCWH; MIM 609136). DNA microarray analysis defined the duplication at 22q11.2q13, including SOX10. Sequencing of the coding region of SOX10 did not reveal any mutations. Our data suggest that SOX10 duplication can cause disorders of sex development and PCWH, supporting the hypothesis that SOX10 toxic gain of function rather than dominant negative activity underlies PCWH.
摘要
当一种疾病的特定组成部分在较晚年龄出现时,遗传综合征的诊断可能会很困难。我们对之前一篇报告[Seeherunvong等人,(2004年);《美国医学遗传学杂志A辑》127:149 - 151]进行了随访,该报告涉及一名患有22q重复和性反转综合征的个体。该个体的表型逐渐发展为包括周围和中枢脱髓鞘、IV型瓦登伯格综合征和先天性巨结肠病(PCWH;MIM 609136)。DNA微阵列分析确定了22q11.2q13区域的重复,包括SOX10。对SOX10编码区的测序未发现任何突变。我们的数据表明,SOX10重复可导致性发育障碍和PCWH,支持了以下假设:SOX10功能获得性毒性而非显性负性活性是PCWH的基础。
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