TK2缺乏症患者的临床与遗传学分析
Clinical and Genetic Analysis of Patients With TK2 Deficiency.
作者信息
Ceballos Francisco, Serrano-Lorenzo Pablo, Bermejo-Guerrero Laura, Blázquez Alberto, Quesada-Espinosa Juan F, Amigo Jorge, Minguez Pablo, Ayuso Carmen, García-Arumí Elena, Muelas Nuria, Jaijo Teresa, Nascimento Andres, Galán-Rodriguez Beatriz, Paradas Carmen, Arenas Joaquín, Carracedo Angel, Martí Ramon, Martín Miguel A, Domínguez-González Cristina
机构信息
From the Spanish Network for Biomedical Research in Rare Diseases (CIBERER) (F.C., P.S.-L., A.B., Jorge Amigo, P.M., C.A., E.G.-A., N.M., T.J., A.N., J. Arenas, A.C., R.M., M.A.M., C.D.-G.); Mitochondrial and Neuromuscular Research Group '12 de Octubre' (P.S.-L., A.B., J. Arenas, M.A.M., C.D.-G.), Hospital Research Institute (imas12); Neurology Department (L.B.-G.), Neuromuscular Disorders Unit, Hospital 12 de Octubre; Genetics Department (J.F.Q.-E., M.A.M.), Hospital Universitario 12 de Octubre, Madrid; Fundación Pública Galega de Medicina Xenómica (FPGMX) (J. Amigo, A.C.); Genetic's Group (J. Amigo, A.C.), Santiago de Compostela Research Institute (IDIS); Medicine Xenómica's Group (J. Amigo, A.C.), Research Center for Molecular Medicine and Chronic Diseases (CIMUS), Santiago de Compostela University (USC); Department of Genetics and Genomics (P.M., C.A.), Instituto de Investigación Sanitaria-Fundación Jiménez Díaz University Hospital; Bioinformatics Unit (P.M.), Health Research Institute-Fundación Jiménez Díaz University Hospital, Universidad Autónoma de Madrid (IIS-FJD, UAM), Madrid; Department of Clinical and Molecular Genetics (E.G.-A.), Valld'Hebron University Hospital; Research Group on Neuromuscular and Mitochondrial Disorders (E.G.-A., R.M.), Vall d'Hebron Research Institut (VHIR), Universitat Autónoma de Barcelona; Neuromuscular Unit (N.M.), Department of Neurology, Hospital Universitari I Politècnic La Fe, Neuromuscular and Ataxias Research Group, Instituto de Investigación Sanitaria La Fe; Department of Genetics (T.J.), Hospital Universitari I Politècnic la Fe de Valencia; Neuromuscular Unit (A.N.), Neurology Department, Sant Joan de Déu Research Institute, Sant Joan de Déu Hospital, Barcelona; Neurology Department (B.G.-R., C.P.), Neuromuscular Disorders Unit, Instituto de Biomedicina de Sevilla, Hospital U. Virgen del Rocío; and Spanish Network for Biomedical Research in Neurodegenerative Diseases (CIBERNED) (C.P.), Madrid, Spain.
出版信息
Neurol Genet. 2024 Mar 25;10(2):e200138. doi: 10.1212/NXG.0000000000200138. eCollection 2024 Apr.
OBJECTIVES
Thymidine kinase 2 deficiency (TK2d) is a rare autosomal recessive disorder that stems from a perturbation of the mitochondrial DNA maintenance. Nucleoside treatment has recently shown promise as a disease-modifying therapy. TK2d was initially associated with rapidly progressive fatal myopathy in children featuring mitochondrial DNA depletion. Subsequently, less severe variants of the disease were described, with onset of symptoms during adolescence or adulthood and associated with the presence of multiple mtDNA deletions. These less severe phenotypes have been reported in only 15% of the approximately 120 patients described worldwide. However, some reports suggest that these juvenile and adult-onset presentations may be more common. The objective of this study was to describe the clinical phenotype in a sample of patients from Spain.
METHODS
This study includes 53 patients harboring biallelic pathogenic variants, compiling data retrospectively from 7 Spanish centers. We analyzed allele frequency, investigated the most recent common ancestor of core haplotypes, and used the Runs of Homozygosity approach to investigate variant coalescence.
RESULTS
Symptom onset distribution revealed that 32 patients (60%) experienced symptoms beyond 12 years of age. Approximately 30% of patients died of respiratory insufficiency, while 56% of surviving patients needed mechanical ventilation. Genetic analysis identified 16 distinct variants in . Two variants, p.Lys202del and p.Thr108Met, exhibited significantly higher prevalence in the Spanish population than that reported in gnomAD database (86-fold and 13-fold, respectively). These variants are estimated to have originated approximately 16.8 generations ago for p.Thr108Met and 95.2 generations ago for p.Lys202del within the Spanish population, with the increase in frequency attributed to various forms of inbreeding. In late-onset cases, 46.9% carried the p.Lys202del variant.
DISCUSSION
The higher frequency of TK2d in Spain can be partially attributed to the increased prevalence of 2 variants and consanguinity. Notably, in 60% of the cohort, the disease was late-onset, emphasizing the potential underdiagnosis of this subgroup of patients in other regions. Raising awareness of this potentially treatable disorder is of utmost importance because early interventions can significantly affect the quality of life and survival of affected individuals.
目的
胸苷激酶2缺乏症(TK2d)是一种罕见的常染色体隐性疾病,源于线粒体DNA维持功能的紊乱。核苷治疗最近显示出有望成为一种改善疾病的疗法。TK2d最初与儿童期快速进展的致命性肌病相关,其特征为线粒体DNA耗竭。随后,发现了病情较轻的该疾病变体,症状在青春期或成年期出现,并与多个线粒体DNA缺失有关。在全球范围内描述的约120例患者中,只有15%报告了这些病情较轻的表型。然而,一些报告表明,这些青少年期和成年期发病的病例可能更为常见。本研究的目的是描述来自西班牙的一组患者的临床表型。
方法
本研究纳入了53例携带双等位基因致病性变体的患者,回顾性收集了来自7个西班牙中心的数据。我们分析了等位基因频率,研究了核心单倍型的最近共同祖先,并使用纯合子片段法研究变体合并情况。
结果
症状发作分布显示,32例患者(60%)在12岁以后出现症状。约30%的患者死于呼吸功能不全,而56%的存活患者需要机械通气。基因分析在……中鉴定出16种不同的变体。两种变体,p.Lys202del和p.Thr108Met,在西班牙人群中的患病率显著高于gnomAD数据库中报告的患病率(分别为86倍和13倍)。据估计,这些变体在西班牙人群中,p.Thr108Met大约在16.8代以前出现,p.Lys202del大约在95.2代以前出现,频率增加归因于各种近亲繁殖形式。在晚发性病例中,46.9%携带p.Lys202del变体。
讨论
西班牙TK2d发病率较高部分可归因于两种变体的患病率增加以及近亲结婚。值得注意的是,在该队列的60%中,疾病为晚发性,这凸显了其他地区该亚组患者可能存在的诊断不足情况。提高对这种可能可治疗疾病的认识至关重要,因为早期干预可显著影响受影响个体的生活质量和生存。
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