十四家系的 Legius 综合征。
Legius syndrome in fourteen families.
机构信息
Department of Human Genetics, Catholic University of Leuven, Belgium.
出版信息
Hum Mutat. 2011 Jan;32(1):E1985-98. doi: 10.1002/humu.21404.
Abstract
Legius syndrome presents as an autosomal dominant condition characterized by café-au-lait macules with or without freckling and sometimes a Noonan-like appearance and/or learning difficulties. It is caused by germline loss-of-function SPRED1 mutations and is a member of the RAS-MAPK pathway syndromes. Most mutations result in a truncated protein and only a few inactivating missense mutations have been reported. Since only a limited number of patients has been reported up until now, the full clinical and mutational spectrum is still unknown. We report mutation data and clinical details in fourteen new families with Legius syndrome. Six novel germline mutations are described. The Trp31Cys mutation is a new pathogenic SPRED1 missense mutation. Clinical details in the 14 families confirmed the absence of neurofibromas, and Lisch nodules, and the absence of a high prevalence of central nervous system tumors. We report white matter T2 hyperintensities on brain MRI scans in 2 patients and a potential association between postaxial polydactyly and Legius syndrome.
摘要
莱格斯综合征表现为常染色体显性遗传疾病,其特征为咖啡牛奶斑伴或不伴雀斑,有时表现为努南样外观和/或学习困难。它是由种系失活 SPRED1 突变引起的,属于 RAS-MAPK 途径综合征。大多数突变导致截短蛋白,只有少数失活错义突变已被报道。由于迄今为止仅报道了有限数量的患者,因此完整的临床和突变谱尚不清楚。我们报告了 14 个新的莱格斯综合征家系的突变数据和临床细节。描述了六个新的种系突变。Trp31Cys 突变是一种新的致病性 SPRED1 错义突变。14 个家系的临床细节证实了神经纤维瘤和神经节细胞瘤的缺失,以及中枢神经系统肿瘤的高发率不存在。我们报告了 2 例患者脑 MRI 扫描上的脑白质 T2 高信号,并且后轴多指与莱格斯综合征之间存在潜在的关联。
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