Human Molecular Genetics Laboratory, National Institute for Biotechnology and Genetic Engineering (NIBGE), Faisalabad, Pakistan.
Department of Immunology, Genetics, and Pathology, Science for Life Laboratory, Uppsala University, Uppsala, Sweden.
Hum Mutat. 2019 Jul;40(7):899-903. doi: 10.1002/humu.23755. Epub 2019 May 24.
Biallelic and pathogenic variants in the RTTN gene, encoding the centrosomal protein Rotatin, are associated with variable degrees of neurodevelopmental abnormalities, microcephaly, and extracranial malformations. To date, no reported case has reached their third decade. Herein, we report on a consanguineous family with three adult members, age 43, 57, and 60 years respectively, with primary microcephaly, developmental delay, primordial dwarfism, and brachydactyly segregating a homozygous splice site variant NM_173630.3:c.5648-5T>A in RTTN. The variant RTTN allele results in a nonhypomorphic skipping of exon 42 and a frameshift [(NP_775901.3:p.Ala1883Glyfs*6)]. Brain MRI of one affected individual showed markedly reduced volume of cerebral lobes and enlarged sulci but without signs of neural migration defects. Our assessment of three adult cases with a biallelic RTTN variant shows that a predicted shortened Rotatin, lacking the C-terminal end, are associated with stationary clinical features into the seventh decade. Furthermore, our report adds brachydactyly to the phenotypic spectrum in this pleiotropic entity.
编码中心体蛋白 Rotatin 的 RTTN 基因中的双等位基因和致病变异与不同程度的神经发育异常、小头畸形和颅外畸形有关。迄今为止,尚无报道的病例达到第三个十年。在此,我们报告了一个近亲家族,有 3 名成年成员,年龄分别为 43、57 和 60 岁,表现为原发性小头畸形、发育迟缓、原始侏儒症和并指,携带 RTTN 基因中的纯合剪接位点变异 NM_173630.3:c.5648-5T>A 。该变异 RTTN 等位基因导致外显子 42 非功能缺失性跳跃和移码 [(NP_775901.3:p.Ala1883Glyfs*6)]。一位受累个体的脑 MRI 显示大脑半球体积明显减小,脑沟扩大,但无神经移行缺陷的迹象。我们对 3 名携带双等位基因 RTTN 变异的成年病例进行评估,结果表明,预测的 Rotatin 缩短,缺乏 C 末端,与进入第 7 个十年的稳定临床特征相关。此外,我们的报告将并指畸形添加到该多效性实体的表型谱中。
