Clinical Hospital Centre Rijeka, Rijeka, Croatia.
Faculty of Medicine, Department of Medical Biology and Genetics, University of Rijeka, Rijeka, Croatia.
Clin Genet. 2024 Dec;106(6):786-787. doi: 10.1111/cge.14623. Epub 2024 Sep 30.
Bosch-Boonstra-Schaaf optic atrophy syndrome (BBSOAS) is an autosomal dominant disease characterized by developmental delay, intellectual disability, and optic atrophy with a variable expression of other clinical features (dysmorphic features, autistic behaviour, corpus callosum hypoplasia and seizures). To date, approximately a hundred cases of the syndrome have been described, with an estimated prevalence of 1 in 100 000-250 000. BBSOAS is caused by the loss of function of the NR2F1 gene (nuclear receptor subfamily 2 group F member 1), which encodes the COUP-TFI (Chicken ovalbumin upstream promotor-transcription factor 1). COUP-TFI functions as a homodimer and is one of the major transcriptional regulators directing cortical arealization, cell differentiation and maturation. Most cases of BBSOAS occur de novo, and one case was previously described in which the disease resulted from gonadal mosaicism. In the present case, we report two sisters with BBSOAS, a novel nonsense mutation in the NR2F1 gene and potential gonadal mosaicism as the cause of this rare disease, making it the second such case described in the literature.
博施-布恩-斯查夫视神经萎缩综合征(BBSOAS)是一种常染色体显性疾病,其特征为发育迟缓、智力残疾和视神经萎缩,伴有其他临床表现(畸形特征、自闭症行为、胼胝体发育不良和癫痫发作)的可变表达。迄今为止,已经描述了大约一百例该综合征,估计患病率为每 10 万至 25 万分之一。BBSOAS 是由 NR2F1 基因(核受体亚家族 2 组 F 成员 1)的功能丧失引起的,该基因编码 COUP-TFI(鸡卵清蛋白上游启动子-转录因子 1)。COUP-TFI 作为同源二聚体发挥作用,是指导皮质区域化、细胞分化和成熟的主要转录调节因子之一。大多数 BBSOAS 病例为新发,先前曾描述过一例该病由性腺嵌合体引起。在本病例中,我们报告了两例患有 BBSOAS 的姐妹,她们的 NR2F1 基因中存在新的无义突变,以及潜在的性腺嵌合体是导致这种罕见疾病的原因,这使其成为文献中描述的第二例此类病例。
