Novel SLC25A4 variant causes mitochondrial depletion rather than Kearns-Sayre syndrome

IF 1.2 4区 医学 Q4 CLINICAL NEUROLOGY Neurosciences Pub Date : 2022-07-01 DOI:10.17712/nsj.2022.3.20220059
J. Finsterer
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Abstract

We have read with interest the article by Zhao et al1 on a 21 years-old male with Kearns-Sayre syndrome (KSS) due to the novel variant c.170G>C in SLC25A4 which led to depletion of the mitochondrial DNA (mtDNA) to 18.7%.1 The patient presented phenotypically with progressive dysarthria starting from age 13, cerebellar atrophy from age 17, and ptosis and ophthalmoparesis from age 19.1 The study is attractive but raises concerns that should be discussed. We disagree with the diagnosis KSS. Kearns-Sayre syndrome is diagnosed based on the phenotype. The prerequisite for the diagnosis is the presence of the 3 main clinical features (progressive external ophthalmoplegia, onset <20y, pigmentary retinopathy) and at least one of the features cerebrospinal fluid (CSF) protein >100mg/dl, cardiac conduction defects, or cerebellar dysfunction.2 Interestingly, the patient did not present with pigmentary retinopathy, or heart block. Additional phenotypic features include hypoacusis, PNS involvement, short stature, growth hormone deficiency, lactic acidosis, facial dysmorphism, hypoparathyroidism, emesis, aortic insufficiency, subaortic septum hypertrophy, right bundle-branch block, and white matter lesions.2 None of these additional features were present in the index patient. It was not possible to assess whether the cerebrospinal fluid (CSF) protein was elevated because reference limits were not given in Table 2.1 Since the patient did not have all three central phenotypic characteristics, and manifested additionally only with cerebellar dysfunction, the diagnosis KSS remains speculative. Since SLC24A4 variants usually cause mitochondrial depletion syndrome (MDS) and KSS is usually due to single mtDNA deletions, single mtDNA duplications, or mtDNA point mutations, the index patient should be diagnosed with MDS, with a KSS-like phenotpye rather than as KSS. Mitochondrial depletion syndrome due to SLC25A4 variants phenotypically manifests with epilepsy, cognitive dysfunction, encephalopathy, cerebral atrophy, white matter lesions, cataract, cardiomyopathy, arterial hypertension, myopathy, or scoliosis.3 Which of these manifestations were found in the index patient? We disagree with the statement in the abstract that KSS is a subtype of progressive external ophthalmoplegia Correspondence
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新的SLC25A4变体导致线粒体耗竭而不是Kearns-Sayre综合征
我们饶有兴趣地阅读了赵等人1关于一名21岁男性的文章,该男性因SLC25A4中的新变体c.170G>c而患有Kearns-Sayre综合征(KSS),导致线粒体DNA(mtDNA)缺失18.7%,以及从19.1岁开始的上睑下垂和眼轻瘫。这项研究很有吸引力,但也引起了人们的关注。我们不同意KSS的诊断。Kearns-Sayre综合征是根据表型诊断的。诊断的先决条件是存在3个主要临床特征(进行性外眼肌麻痹,发作100mg/dl,心脏传导缺陷或小脑功能障碍。2有趣的是,患者没有出现色素性视网膜病变或心脏传导阻滞。其他表型特征包括听力减退、PNS受累、身材矮小、生长激素缺乏、乳酸酸中毒、面部畸形、甲状旁腺功能减退、呕吐、主动脉瓣功能不全、主动脉隔膜肥大、右束支传导阻滞和白质病变。2这些额外特征在指数患者中均未出现。由于表2.1中没有给出参考限值,因此无法评估脑脊液(CSF)蛋白是否升高。由于患者不具有所有三个中心表型特征,并且仅表现为小脑功能障碍,因此诊断KSS仍然是推测性的。由于SLC24A4变异体通常会导致线粒体耗竭综合征(MDS),而KSS通常是由单个mtDNA缺失、单个mtDNA重复或mtDNA点突变引起的,因此指数患者应被诊断为MDS,具有KSS样表型,而不是KSS。SLC25A4变体引起的线粒体耗竭综合征表现为癫痫、认知功能障碍、脑病、脑萎缩、白质病变、白内障、心肌病、动脉高压、肌病或脊柱侧弯。3在指标患者中发现了以下哪种表现?我们不同意抽象的说法,即KSS是进行性外眼肌麻痹对应症的一种亚型
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来源期刊
Neurosciences
Neurosciences 医学-临床神经学
CiteScore
1.40
自引率
0.00%
发文量
54
审稿时长
4.5 months
期刊介绍: Neurosciences is an open access, peer-reviewed, quarterly publication. Authors are invited to submit for publication articles reporting original work related to the nervous system, e.g., neurology, neurophysiology, neuroradiology, neurosurgery, neurorehabilitation, neurooncology, neuropsychiatry, and neurogenetics, etc. Basic research withclear clinical implications will also be considered. Review articles of current interest and high standard are welcomed for consideration. Prospective workshould not be backdated. There are also sections for Case Reports, Brief Communication, Correspondence, and medical news items. To promote continuous education, training, and learning, we include Clinical Images and MCQ’s. Highlights of international and regional meetings of interest, and specialized supplements will also be considered. All submissions must conform to the Uniform Requirements.
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