Institute of Human Genetics, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
Department of Neurology, Program in Neurogenetics, David Geffen School of Medicine, University of California Los Angeles, Los Angeles, CA, USA.
Eur J Hum Genet. 2024 May;32(5):558-566. doi: 10.1038/s41431-024-01563-5. Epub 2024 Feb 19.
Biallelic loss-of-function variants in TBC1D2B have been reported in five subjects with cognitive impairment and seizures with or without gingival overgrowth. TBC1D2B belongs to the family of Tre2-Bub2-Cdc16 (TBC)-domain containing RAB-specific GTPase activating proteins (TBC/RABGAPs). Here, we report five new subjects with biallelic TBC1D2B variants, including two siblings, and delineate the molecular and clinical features in the ten subjects known to date. One of the newly reported subjects was compound heterozygous for the TBC1D2B variants c.2584C>T; p.(Arg862Cys) and c.2758C>T; p.(Arg920*). In subject-derived fibroblasts, TBC1D2B mRNA level was similar to control cells, while the TBC1D2B protein amount was reduced by about half. In one of two siblings with a novel c.360+1G>T splice site variant, TBC1D2B transcript analysis revealed aberrantly spliced mRNAs and a drastically reduced TBC1D2B mRNA level in leukocytes. The molecular spectrum included 12 different TBC1D2B variants: seven nonsense, three frameshifts, one splice site, and one missense variant. Out of ten subjects, three had fibrous dysplasia of the mandible, two of which were diagnosed as cherubism. Most subjects developed gingival overgrowth. Half of the subjects had developmental delay. Seizures occurred in 80% of the subjects. Six subjects showed a progressive disease with mental deterioration. Brain imaging revealed cerebral and/or cerebellar atrophy with or without lateral ventricle dilatation. The TBC1D2B disorder is a progressive neurological disease with gingival overgrowth and abnormal mandible morphology. As TBC1D2B has been shown to positively regulate autophagy, defects in autophagy and the endolysosomal system could be associated with neuronal dysfunction and the neurodegenerative disease in the affected individuals.
TBC1D2B 的双等位基因功能丧失变异已在 5 名认知障碍伴或不伴牙龈过度生长的癫痫患者中报道。TBC1D2B 属于 Tre2-Bub2-Cdc16(TBC)-结构域包含的 RAB 特异性 GTP 酶激活蛋白(TBC/RABGAPs)家族。在这里,我们报告了 5 名新的 TBC1D2B 双等位基因突变患者,包括 2 名同胞,并描绘了迄今为止已知的 10 名患者的分子和临床特征。新报告的患者之一为 TBC1D2B 变异 c.2584C>T;p.(Arg862Cys) 和 c.2758C>T;p.(Arg920*) 的复合杂合子。在源自受检者的成纤维细胞中,TBC1D2B mRNA 水平与对照细胞相似,而 TBC1D2B 蛋白量减少了约一半。在一对同胞中,其中一人携带新的 c.360+1G>T 剪接位点变异,TBC1D2B 转录分析显示异常剪接的 mRNA 和白细胞中 TBC1D2B mRNA 水平显著降低。分子谱包括 12 种不同的 TBC1D2B 变异:7 种无义变异,3 种移码变异,1 种剪接位点变异和 1 种错义变异。在 10 名患者中,有 3 名患有下颌纤维结构不良,其中 2 名被诊断为 cherubism。大多数患者出现牙龈过度生长。一半的患者有发育迟缓。80%的患者出现癫痫发作。6 名患者表现出进行性疾病,伴有精神恶化。脑成像显示大脑和/或小脑萎缩,伴有或不伴有侧脑室扩张。TBC1D2B 疾病是一种进行性神经疾病,伴有牙龈过度生长和下颌异常形态。由于 TBC1D2B 已被证明正向调节自噬,因此自噬和内溶酶体系统的缺陷可能与受影响个体的神经元功能障碍和神经退行性疾病有关。
