Armirola-Ricaurte Camila, Morant Laura, Adant Isabelle, Hamed Sherifa Ahmed, Pipis Menelaos, Efthymiou Stephanie, Amor-Barris Silvia, Atkinson Derek, Van de Vondel Liedewei, Tomic Aleksandra, de Vriendt Els, Zuchner Stephan, Ghesquiere Bart, Hanna Michael, Houlden Henry, Lunn Michael P, Reilly Mary M, Rasic Vedrana Milic, Jordanova Albena
medRxiv. 2024 Jul 4:2024.07.03.24309787. doi: 10.1101/2024.07.03.24309787.
Defects in mitochondrial dynamics are a common cause of Charcot-Marie-Tooth disease (CMT), while primary deficiencies in the mitochondrial respiratory chain (MRC) are rare and atypical for this etiology. This study aims to report as a novel CMT-causing gene. This gene encodes an assembly factor of mitochondrial Complex IV (CIV) that translocates the C-terminal tail of MTCO2 across the mitochondrial inner membrane. Exome sequencing was performed in four affected individuals. The patients and available family members underwent thorough neurological and electrophysiological assessment. The impact of one of the identified variants on splicing, protein levels, and mitochondrial bioenergetics was investigated in patient-derived lymphoblasts. The functionality of the mutant protein was assessed using a Proteinase K protection assay and immunoblotting. Neuronal relevance of COX18 was assessed in a knockdown model. Exome sequencing coupled with homozygosity mapping revealed a homozygous splice variant c.435-6A>G in in two siblings with early-onset progressive axonal sensory-motor peripheral neuropathy. By querying external databases, we identified two additional families with rare deleterious biallelic variants in . All affected individuals presented with axonal CMT and some patients also exhibited central nervous system symptoms, such as dystonia and spasticity. Functional characterization of the c.435-6A>G variant demonstrated that it leads to the expression of an alternative transcript that lacks exon 2, resulting in a stable but defective COX18 isoform. The mutant protein impairs CIV assembly and activity, leading to a reduction in mitochondrial membrane potential. Downregulation of the homolog in displayed signs of neurodegeneration, including locomotor deficit and progressive axonal degeneration of sensory neurons. Our study presents genetic and functional evidence that supports as a newly identified gene candidate for autosomal recessive axonal CMT with or without central nervous system involvement. These findings emphasize the significance of peripheral neuropathy within the spectrum of primary mitochondrial disorders and the role of mitochondrial CIV in the development of CMT. Our research has important implications for the diagnostic workup of CMT patients.
线粒体动力学缺陷是夏科-马里-图斯病(CMT)的常见病因,而线粒体呼吸链(MRC)的原发性缺陷在该病因中罕见且不典型。本研究旨在报告一个新的导致CMT的基因。该基因编码线粒体复合物IV(CIV)的一个组装因子,它将MTCO2的C末端尾巴转运穿过线粒体内膜。对四名受影响个体进行了外显子组测序。对患者及可用的家庭成员进行了全面的神经学和电生理学评估。在患者来源的淋巴母细胞中研究了其中一个已鉴定变体对剪接、蛋白质水平和线粒体生物能量学的影响。使用蛋白酶K保护试验和免疫印迹评估突变蛋白的功能。在敲低模型中评估了COX18的神经元相关性。外显子组测序结合纯合性定位在两名患有早发性进行性轴索性感觉运动性周围神经病的兄弟姐妹中发现了一个纯合剪接变体c.435-6A>G。通过查询外部数据库,我们在另外两个家族中鉴定出了罕见的有害双等位基因变体。所有受影响个体均表现为轴索性CMT,一些患者还表现出中枢神经系统症状,如肌张力障碍和痉挛。对c.435-6A>G变体的功能表征表明,它导致一种缺乏外显子2的替代转录本的表达,产生一种稳定但有缺陷的COX18异构体。突变蛋白损害CIV的组装和活性,导致线粒体膜电位降低。在果蝇中下调同源物显示出神经退行性变的迹象,包括运动缺陷和感觉神经元的进行性轴索变性。我们的研究提供了遗传和功能证据,支持将其作为常染色体隐性轴索性CMT(伴或不伴中枢神经系统受累)的新鉴定基因候选物。这些发现强调了原发性线粒体疾病范围内周围神经病的重要性以及线粒体CIV在CMT发展中的作用。我们的研究对CMT患者的诊断检查具有重要意义。
