A novel electron transfer flavoprotein dehydrogenase (ETFDH) gene mutation identified in a newborn with glutaric acidemia type II: a case report of a Chinese family

Ou, Mingcai; Zhu, Lin; Zhang, Yong; Zhang, Yaguo; Zhou, Jia; Chen, Xuelian; Yang, Lijuan; Li, Ting; Su, Xingyue; Hu, Qi; Wang, Wenjun

doi:10.1186/s12881-020-00995-2

Cited by 10 publications

(9 citation statements)

References 22 publications

(29 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In our study, patient 4 with compound heterozygous variants, a frameshift mutation c.582_583insTA (p.P196T fs * 17) and a missense variant c.295C>T (p.R99C) had a relatively average age of onset and typical clinical picture of LOMADD. Nevertheless, previous reports reveal that patients with heterozygous frameshift and missense mutations appear to have an earlier age of onset than those with heterozygous missense mutations (32,(34)(35)(36)(37). Additionally, they frequently exhibit episodes of vomiting, drowsiness, appetite loss, asthenia, and acetonemic breath (32,(34)(35)(36)(37), none of which are prevalent in LOMADD.…”

Section: Discussionmentioning

confidence: 96%

Clinical Presentations and Genetic Characteristics of Late-Onset MADD Due to ETFDH Mutations in Five Patients: A Case Series

Tang

Gao

et al. 2021

Front. Neurol.

View full text Add to dashboard Cite

Background: Late-onset multiple acyl-CoA dehydrogenase deficiency (LO-MADD) describes a curable autosomal recessive genetic disease caused by ETFDH mutations that result in defects in ETF-ubiquinone oxidoreductase. Almost all patients are responsive to riboflavin. This study describes the clinical presentations and genetic characteristics of five LO-MADD patients.Methods: From 2018 to 2021, we collected clinical and genetic data on five patients diagnosed with LO-MADD at our hospital and retrospectively analyzed their clinical characteristics, laboratory examination, electromyography, muscle biopsy, genetic analysis, and outcome data.Results: This study included three males and two females with mean onset age of 37.8 years. Fluctuating exercise intolerance was the most common presentation. Serum creatine kinase (CK) levels were significantly elevated in all patients, and plasma acylcarnitine profiles revealed an increase in long-chain acylcarnitine species in three cases. The urinary organic acid study revealed a high level of hydroxyglutaric acid in all patients. Electrophysiology demonstrated myogenic impairment. Muscle biopsies revealed lipid storage myopathy. Molecular analysis identified nine mutations (three novels and six reported) in ETFDH. Exercise intolerance and muscle weakness were dramatically improved in all patients treated with riboflavin (100 mg) daily following diagnosis.Conclusions: LO-MADD is caused by ETFDH variants and responds well to riboflavin. Three novel ETFDH pathogenic variants were identified, expanding their spectrum in the Chinese population and facilitating future interpretation and analysis of ETFDH mutations.

show abstract

Section: Discussionmentioning

confidence: 96%

Clinical Presentations and Genetic Characteristics of Late-Onset MADD Due to ETFDH Mutations in Five Patients: A Case Series

Tang

Gao

et al. 2021

Front. Neurol.

View full text Add to dashboard Cite

show abstract

“…MADD is a rare, potentially treatable β-oxidation disorder with three main subtypes: types I/II represent early onset in the neonatal period or infancy and type III represents the late onset of the disease [3,22].…”

Section: Discussionmentioning

confidence: 99%

Multiple Acyl-CoA Dehydrogenase Deficiency with Variable Presentation Due to a Homozygous Mutation in a Bedouin Tribe

Staretz‐Chacham

Amar

Almashanu

et al. 2021

Genes

View full text Add to dashboard Cite

Multiple acyl-CoA dehydrogenase deficiency (MADD) is a fatty acid and amino acid oxidation defect caused by a deficiency of the electron-transfer flavoprotein (ETF) or the electron-transfer flavoprotein dehydrogenase (ETFDH). There are three phenotypes of the disease, two neonatal forms and one late-onset. Previous studies have suggested that there is a phenotype–genotype correlation. We report on six patients from a single Bedouin tribe, five of whom were sequenced and found to be homozygous to the same variant in the ETFDH gene, with variable severity and age of presentation. The variant, NM_004453.3 (ETFDH): c.524G>A, p.(R175H), was previously recognized as pathogenic, although it has not been reported in the literature in a homozygous state before. R175H is located near the FAD binding site, likely affecting the affinity of FAD for EFT:QO. The single homozygous ETFDH pathogenic variant was found to be causing MADD in this cohort with an unexpectedly variable severity of presentation. The difference in severity could partly be explained by early diagnosis via newborn screening and early treatment with the FAD precursor riboflavin, highlighting the importance of early detection by newborn screening.

show abstract

“…Multiple studies have demonstrated that patients with MADD generally have mutations in ETFA, ETFB or ETFDH genes [ 11 , 12 , 13 ]. According to the Human Gene Mutation Database (HGMD), over 190 different variants of ETFDH have been reported so far and most of them are associated with the late-onset form of GA-II [ 14 , 15 , 16 ]. The majority of patients presented with the late-onset form are responsive to riboflavin therapy, but the molecular mechanism remains elusive.…”

Section: Introductionmentioning

confidence: 99%

Clinical, Biochemical, and Genetic Heterogeneity in Glutaric Aciduria Type II Patients

Ali

Almesmari

Dhahouri

et al. 2021

Genes

View full text Add to dashboard Cite

The variants of electron transfer flavoprotein (ETFA, ETFB) and ETF dehydrogenase (ETFDH) are the leading cause of glutaric aciduria type II (GA-II). In this study, we identified 13 patients harboring six variants of two genes associated with GA-II. Out of the six variants, four were missense, and two were frameshift mutations. A missense variant (ETFDH:p.Gln269His) was observed in a homozygous state in nine patients. Among nine patients, three had experienced metabolic crises with recurrent vomiting, abdominal pain, and nausea. In one patient with persistent metabolic acidosis, hypoglycemia, and a high anion gap, the ETFDH:p.Gly472Arg, and ETFB:p.Pro94Thrfs*8 variants were identified in a homozygous, and heterozygous state, respectively. A missense variant ETFDH: p.Ser442Leu was detected in a homozygous state in one patient with metabolic acidosis, hypoglycemia, hyperammonemia and liver dysfunction. The ETFDH:p.Arg41Leu, and ETFB:p.Ile346Phefs*19 variants were observed in a homozygous state in one patient each. Both these variants have not been reported so far. In silico approaches were used to evaluate the pathogenicity and structural changes linked with these six variants. Overall, the results indicate the importance of a newborn screening program and genetic investigations for patients with GA-II. Moreover, careful interpretation and correlation of variants of uncertain significance with clinical and biochemical findings are needed to confirm the pathogenicity of such variants.

show abstract

A novel electron transfer flavoprotein dehydrogenase (ETFDH) gene mutation identified in a newborn with glutaric acidemia type II: a case report of a Chinese family

Cited by 10 publications

References 22 publications

Clinical Presentations and Genetic Characteristics of Late-Onset MADD Due to ETFDH Mutations in Five Patients: A Case Series

Clinical Presentations and Genetic Characteristics of Late-Onset MADD Due to ETFDH Mutations in Five Patients: A Case Series

Multiple Acyl-CoA Dehydrogenase Deficiency with Variable Presentation Due to a Homozygous Mutation in a Bedouin Tribe

Clinical, Biochemical, and Genetic Heterogeneity in Glutaric Aciduria Type II Patients

Contact Info

Product

Resources

About