Journal article

Clinical and biochemical distinctions for a metabolite repair disorder caused by NAXD or NAXE deficiency

NJ Van Bergen, AS Walvekar, M Patraskaki, T Sikora, CL Linster, J Christodoulou

Journal of Inherited Metabolic Disease | WILEY | Published : 2022

DOI: 10.1002/jimd.12541

Download PDF

Abstract

The central cofactors NAD(P)H are prone to damage by hydration, resulting in formation of redox-inactive derivatives designated NAD(P)HX. The highly conserved enzymes NAD(P)HX dehydratase (NAXD) and NAD(P)HX epimerase (NAXE) function to repair intracellular NAD(P)HX. Recently, pathogenic variants in both the NAXD and NAXE genes were associated with rapid deterioration and death after an otherwise trivial fever, infection, or illness in young patients. As more patients are identified, distinct clinical features are emerging depending on the location of the pathogenic variant. In this review, we carefully catalogued the clinical features of all published NAXD deficiency patients and found dist..

View full abstract

Grants

Awarded by Murdoch Children's Research Institute

Funding Acknowledgements

Luxembourg National Research Fund, Grant/Award Number: C18/BM/12661133; The Royal Children's Hospital Foundation; Murdoch Children's Research Institute; Mito Foundation; State Government of Victoria's Operational Infrastructure Support Program; Juniclair Foundation

Citation metrics

17Scopus
6Web of Science
18Dimensions

Keywords

Research & Experimental Medicine
Endocrinology & Metabolism
Neurosciences
3202 Clinical Sciences
31 Biological Sciences
Musculoskeletal
Febrile Illness
Metabolite Repair
Skin Lesions
System
Mutations
Science & Technology
Genetics & Heredity
Naxe Deficiency
Rare Diseases
Neurodegenerative
Life Sciences & Biomedicine
Nadh
2.1 Biological and Endogenous Factors
Naxd Deficiency
Metabolism
Genetics
32 Biomedical and Clinical Sciences
Medicine, Research & Experimental
Neurodegeneration