Clinical Genetic Service, Department of Health, University of Hong Kong, HKSAR, Hong Kong.
Clinical Genetic Service, Department of Health, University of Hong Kong, HKSAR, Hong Kong.
Eur J Med Genet. 2021 Jan;64(1):104107. doi: 10.1016/j.ejmg.2020.104107. Epub 2020 Nov 23.
Bainbridge-Ropers syndrome (BRPS) [OMIM#615485] is a neurodevelopmental disorder, characterized by delayed psychomotor development with generalized hypotonia, intellectual disability with poor or absent speech, feeding difficulties, growth failure, specific craniofacial and minor skeletal features. It was firstly reported in 2013 by Bainbridge et al., who observed a group of individuals sharing overlapping features with Bohring-Opitz syndrome which were caused by pathogenic variant in ASXL1, who indeed carried truncating mutations in ASXL3. To date, 33 cases were described in the literature. BRPS is caused by loss-of-function mutations in ASXL3 which are mostly located in two mutational cluster regions (MCR). The exact molecular mechanism of these mutations resulting in the disease phenotype is still uncertain due to the observation of LOF mutations in healthy population. Here, we report four individuals with BRPS carrying de novo LOF mutations in ASXL3, comparing and summarizing the clinical phenotype of all BRPS reported so far. Furthermore, we try to dissect the genotype-phenotype correlation among the two well reported MCRs in all BRPS from the literature.
贝恩布里奇-罗珀斯综合征(BRPS)[OMIM#615485] 是一种神经发育障碍,其特征为精神运动发育迟缓伴全身明显张力减退、言语障碍伴智力障碍、喂养困难、生长不良、特殊颅面及小骨骼特征。该疾病由 Bainbridge 等人于 2013 年首次报道,他们观察到一组个体具有与 Bohring-Opitz 综合征重叠的特征,后者由 ASXL1 中的致病性变异引起,而实际上 ASXL3 携带截断突变。迄今为止,文献中已有 33 例报道。BRPS 是由 ASXL3 的功能丧失突变引起的,这些突变主要位于两个突变簇区域(MCR)。由于在健康人群中观察到 LOF 突变,这些突变导致疾病表型的确切分子机制仍不确定。在此,我们报道了 4 例携带 ASXL3 新生 LOF 突变的 BRPS 患者,比较并总结了迄今为止所有报道的 BRPS 的临床表型。此外,我们还尝试从文献中分析所有 BRPS 中两个报道较多的 MCR 之间的基因型-表型相关性。
