Doğulu Neslihan, Köse Engin, Ceylaner Serdar, Kasapkara Çiğdem Seher, Bozaci Ayşe Ergul, Oncul Ummuhan, Eminoğlu Fatma Tuba
Department of Pediatric Metabolism, Ankara University Faculty of Medicine, Ankara, Turkey.
Intergen Genetics and Rare Diseases Diagnosis Research and Application Center, Ankara, Turkey.
Mol Syndromol. 2024 Dec;15(6):450-463. doi: 10.1159/000539034. Epub 2024 Jun 17.
Mitochondrial DNA depletion syndromes (MDDSs) are a group of clinically and genetically heterogeneous disorders. In the present study, we aimed to investigate the frequency of MDDS in children under the age of 5 years with suspected mitochondrial hepatopathy and to evaluate this group of patients using MDDS gene panel and clinical exome sequencing (CES) genetic analysis methods.
Patients under 5 years of age who were clinically suspected to have mitochondrial hepatopathy and had neonatal acute liver failure, hepatic steatohepatitis, cholestasis, or cirrhosis with chronic liver failure of insidious onset were included.
Forty patients (20 female, 50%) were enrolled, with a median age of 102 [57-263.8] days. Icteric appearance was identified in 28 (70%) of the patients, hepatomegaly in 27 (67.5%), splenomegaly in 10 (25.0%), and hypotonicity in 10 (25.0%); moreover, elevated international normalized ratio was detected in 77.5%, cholestasis in 77.5%, and elevated lactate levels in 62.5%. Molecular genetic diagnosis was made in 9 patients (22.5%) with the MDDS gene panel and in 17 (42.5%) patients with the CES analysis. All patients diagnosed with MDDS had a history of parental consanguinity, while the rate in those without MDDS was 54.8% ( = 0.012). High lactate levels were identified in all those with MDDS, but in only 51.6% of those without MDDS ( = 0.020).
Present study revealed that demographic findings and laboratory assessments are insufficient to diagnose genetically inherited diseases in children presenting with hepatic involvement. While one-fifth of the patients with suspected mitochondrial hepatopathies were diagnosed with MDDS, it is revealed that around half of patients can be diagnosed with CES panel.
线粒体DNA耗竭综合征(MDDSs)是一组临床和遗传异质性疾病。在本研究中,我们旨在调查5岁以下疑似线粒体肝病儿童中MDDS的发生率,并使用MDDS基因检测板和临床外显子组测序(CES)遗传分析方法对该组患者进行评估。
纳入临床疑似患有线粒体肝病且有新生儿急性肝衰竭、肝脂肪性肝炎、胆汁淤积或隐匿性发作的慢性肝衰竭伴肝硬化的5岁以下患者。
共纳入40例患者(20例女性,占50%),中位年龄为102[57 - 263.8]天。28例(70%)患者有黄疸表现,27例(67.5%)有肝肿大,10例(25.0%)有脾肿大,10例(25.0%)有肌张力减退;此外,77.5%检测到国际标准化比值升高,77.5%有胆汁淤积,62.5%有乳酸水平升高。使用MDDS基因检测板对9例(22.5%)患者进行了分子遗传学诊断,使用CES分析对17例(42.5%)患者进行了诊断。所有诊断为MDDS的患者都有近亲结婚史,而未患MDDS的患者中这一比例为54.8%(P = 0.012)。所有患MDDS的患者乳酸水平都很高,但未患MDDS的患者中只有51.6%如此(P = 0.020)。
本研究表明,人口统计学结果和实验室评估不足以诊断有肝脏受累表现的儿童遗传性疾病。虽然五分之一疑似线粒体肝病的患者被诊断为MDDS,但结果显示约一半患者可通过CES检测板诊断。
