Natural history of deoxyguanosine kinase deficiency

IF 3.7 2区 生物学 Q2 ENDOCRINOLOGY & METABOLISM Molecular genetics and metabolism Pub Date : 2024-07-24 DOI:10.1016/j.ymgme.2024.108554
Nandaki Keshavan , Shamima Rahman
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Abstract

Background and objectives

Deoxyguanosine kinase deficiency is one genetic cause of mtDNA depletion syndrome. Its major phenotypes include neonatal/infantile-onset hepatocerebral disease, isolated hepatic disease and myopathic disease. In this retrospective study, we seek to describe the natural history of deoxyguanosine kinase deficiency and identify any genotype-phenotype correlations.

Methods

Retrospective literature search and collation of data from genetically confirmed cases of deoxyguanosine kinase deficiency.

Results

173 cases of DGUOK deficiency were identified. Neonatal/infantile-onset hepatocerebral disease accounted for 128 (74%) of cases. Isolated liver disease was seen in 36 (21%) and myopathic disease in 9 (5%) of cases. The most frequently involved systems were liver (98%), brain (75%), growth (46%) and gastrointestinal tract (26%). Infantile-onset disease typically presented with cholestatic jaundice and lactic acidosis. Neurological involvement included hypotonia, nystagmus and developmental delay with MRI brain abnormalities in about half of cases. Missense variants accounted for 48% of all pathogenic variants while variants resulting in truncated transcripts accounted for 39%. Prognosis was poor, especially for neonatal/ infantile-onset hepatocerebral disease for which 1 year survival was 11%. Twenty-three patients received liver transplants, of whom 12 died within 2 years of transplant. Patients with two truncating variants had a higher risk of death and were more likely to have the neonatal/infantile-onset hepatocerebral disease phenotype. No blood biomarker predictive of neurological involvement was identified. Earlier onset correlated with increased mortality.

Conclusions

There is a narrow window for therapeutic intervention. For the hepatocerebral disease phenotype, median age of onset was 1 month while the median age of death was 6.5 months implying rapid disease progression.

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脱氧鸟苷激酶缺乏症的自然史
脱氧鸟苷激酶缺乏症是mtDNA耗竭综合征的一种遗传病因。其主要表现型包括新生儿/幼年期肝脑病、孤立性肝病和肌病。在这项回顾性研究中,我们试图描述脱氧鸟苷激酶缺乏症的自然史,并确定基因型与表型之间的相关性。回顾性文献检索和整理经基因证实的脱氧鸟苷激酶缺乏症病例的数据。共发现 173 例脱氧鸟苷激酶缺乏症病例。新生儿/婴儿期发病的肝脑疾病占128例(74%)。36例(21%)病例出现孤立性肝病,9例(5%)病例出现肌病。最常受累的系统是肝脏(98%)、大脑(75%)、生长(46%)和胃肠道(26%)。婴儿期发病的典型症状是胆汁淤积性黄疸和乳酸性酸中毒。神经系统受累包括肌张力低下、眼球震颤和发育迟缓,约半数病例出现磁共振成像脑部异常。在所有致病变异中,错义变异占 48%,而导致转录本截短的变异占 39%。预后很差,尤其是新生儿/婴儿期发病的肝脑病,1年存活率仅为11%。23名患者接受了肝移植,其中12人在移植后2年内死亡。有两个截短变体的患者死亡风险更高,更有可能出现新生儿/婴儿型肝脑疾病表型。没有发现可预测神经系统受累的血液生物标志物。发病时间越早,死亡率越高。治疗干预的窗口很窄。肝脑疾病表型的中位发病年龄为1个月,而中位死亡年龄为6.5个月,这意味着疾病进展迅速。
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来源期刊
Molecular genetics and metabolism
Molecular genetics and metabolism 生物-生化与分子生物学
CiteScore
5.90
自引率
7.90%
发文量
621
审稿时长
34 days
期刊介绍: Molecular Genetics and Metabolism contributes to the understanding of the metabolic and molecular basis of disease. This peer reviewed journal publishes articles describing investigations that use the tools of biochemical genetics and molecular genetics for studies of normal and disease states in humans and animal models.
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