[A case of combined oxidative phosphorylation deficiency 32 caused by MRPS34 gene variation and literature review].

M X Shen, X N Ji, F Wu, Y Y Gao, S Feng, L N Xie, P Zheng, Y Y Mao, Q Chen
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Abstract

Objective: To investigate the clinical features and genetic features of combined oxidative phosphorylation deficiency 32 (COXPD32) caused by MRPS34 gene variation. Methods: The clinical data and genetic test of a child with COXPD32 hospitalized in the Department of Neurology, Children's Hospital, Capital Institute of Pediatrics in March 2021 were extracted and analyzed. A literature search was implemented using Wanfang, China biology medicine disc, China national knowledge infrastructure, ClinVar, human gene mutation database (HGMD) and Pubmed databases with the key words "MRPS34" "MRPS34 gene" and "combined oxidative phosphorylation deficiency 32" (up to February 2023). Clinical and genetic features of COXPD32 were summarized. Results: A boy aged 1 year and 9 months was admitted due to developmental delay. He showed mental and motor retardation, and was below the 3rd percentile for height, weight, and head circumference of children of the same age and gender. He had poor eye contact, esotropia, flat nasal bridge, limbs hypotonia, holding instability and tremors. In addition, Grade Ⅲ/6 systolic murmur were heard at left sternal border. Arterial blood gases suggested that severe metabolic acidosis with lactic acidosis. Brain magnetic resonance imaging (MRI) showed multiple symmetrical abnormal signals in the bilateral thalamus, midbrain, pons and medulla oblongata. Echocardiography showed atrial septal defect. Genetic testing identified the patient as a compound heterozygous variation of MRPS34 gene, c.580C>T (p.Gln194Ter) and c.94C>T (p.Gln32Ter), with c.580C>T being the first report and a diagnosis of COXPD32. His parents carried a heterozygous variant, respectively. The child improved after treatment with energy support, acidosis correction, and "cocktail" therapy (vitaminB1, vitaminB2, vitaminB6, vitaminC and coenzyme Q10). A total of 8 cases with COXPD32 were collected through 2 English literature reviews and this study. Among the 8 patients, 7 cases had onset during infancy and 1 was unknown, all had developmental delay or regression, 7 cases had feeding difficulty or dysphagia, followed by dystonia, lactic acidosis, ocular symptoms, microcephaly, constipation and dysmorphic facies(mild coarsening of facial features, small forehead, anterior hairline extending onto forehead,high and narrow palate, thick gums, short columella, and synophrys), 2 cases died of respiratory and circulatory failure, and 6 were still alive at the time of reporting, with an age range of 2 to 34 years. Blood and (or) cerebrospinal fluid lactate were elevated in all 8 patients. MRI in 7 cases manifested symmetrical abnormal signals in the brainstem, thalamus, and (or) basal ganglia. Urine organic acid test were all normal but 1 patient had alanine elevation. Five patients underwent respiratory chain enzyme activity testing, and all had varying degrees of enzyme activity reduction. Six variants were identified, 6 patients were homozygous variants, with c.322-10G>A was present in 4 patients from 2 families and 2 compound heterozygous variants. Conclusions: The clinical phenotype of COXPD32 is highly heterogenous and the severity of the disease varies from development delay, feeding difficulty, dystonia, high lactic acid, ocular symptoms and reduced mitochondrial respiratory chain enzyme activity in mild cases, which may survive into adulthood, to rapid death due to respiratory and circulatory failure in severe cases. COXPD32 needs to be considered in cases of unexplained acidosis, hyperlactatemia, feeding difficulties, development delay or regression, ocular symptoms, respiratory and circulatory failure, and symmetrical abnormal signals in the brainstem, thalamus, and (or) basal ganglia, and genetic testing can clarify the diagnosis.

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【MRPS34基因变异引起的合并氧化磷酸化缺陷32 1例及文献复习】。
目的:探讨MRPS34基因变异引起的联合氧化磷酸化缺陷32 (COXPD32)的临床特征和遗传特征。方法:提取2021年3月首都儿科研究所儿童医院神经内科收治的1例COXPD32患儿的临床资料及基因检测资料进行分析。使用万方、中国生物医学光盘、中国国家知识基础设施、ClinVar、人类基因突变数据库(HGMD)和Pubmed数据库进行文献检索,检索关键词为“MRPS34”、“MRPS34基因”和“联合氧化磷酸化缺陷32”(截止至2023年2月)。总结了COXPD32的临床和遗传学特征。结果:1例1岁9个月男童因发育迟缓入院。他表现出智力和运动迟缓,身高、体重和头围低于同年龄和性别儿童的第3百分位。患者目光接触不良,内斜视,鼻梁扁平,四肢强直,持稳不稳,震颤。此外,左侧胸骨边界可听到Ⅲ/6级收缩期杂音。动脉血气提示严重代谢性酸中毒伴乳酸性酸中毒。脑磁共振成像(MRI)显示双侧丘脑、中脑、脑桥和延髓多发对称异常信号。超声心动图显示房间隔缺损。基因检测发现患者为MRPS34基因复合杂合变异,c.580C>T (p.Gln194Ter)和c.94C>T (p.Gln32Ter),其中c.580C>T为首次报道并诊断为COXPD32。他的父母分别携带一种杂合变体。经能量支持、酸中毒矫正和“鸡尾酒疗法”(维生素b1、维生素b2、维生素b6、维生素c和辅酶Q10)治疗后,患儿病情好转。通过2篇英文文献综述和本研究共收集到8例COXPD32。8例患者中,7例发病于婴儿期,1例发病原因不明,均有发育迟缓或倒退,7例出现进食困难或吞咽困难,其次为肌痉挛、乳酸性酸中毒、眼部症状、小头畸形、便秘及畸形相(面部特征轻度粗化、额头小、发际线前伸至额头、上颚高窄、牙龈厚、小柱短、颏部),2例死于呼吸和循环衰竭。其中6人在报告时仍然活着,年龄在2至34岁之间。8例患者血和(或)脑脊液乳酸均升高。7例MRI表现为脑干、丘脑和(或)基底节区对称异常信号。尿有机酸试验均正常,但有1例丙氨酸升高。5例患者行呼吸链酶活性检测,均有不同程度的酶活性降低。共鉴定出6个变异,6例为纯合变异,2个家族的4例患者存在c.322-10G>A, 2例为复合杂合变异。结论:COXPD32临床表型具有高度异质性,病情轻重不一,轻者可发育迟缓、进食困难、肌张力障碍、高乳酸、眼部症状、线粒体呼吸链酶活性降低,可存活至成年期,重者可因呼吸和循环衰竭而迅速死亡。在不明原因酸中毒、高乳酸血症、喂养困难、发育迟缓或倒退、眼部症状、呼吸和循环衰竭,以及脑干、丘脑和(或)基底节区对称异常信号的情况下,需要考虑COXPD32,基因检测可以明确诊断。
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