| Literature DB >> 31132363 |
Peter Huppke1, Eike Wegener2, Jonathan Gilley3, Carlo Angeletti4, Ingo Kurth5, Joost P H Drenth6, Christine Stadelmann7, Alonso Barrantes-Freer8, Wolfgang Brück9, Holger Thiele10, Peter Nürnberg11, Jutta Gärtner12, Giuseppe Orsomando13, Michael P Coleman14.
Abstract
We identified a homozygous missense mutation in the gene encoding NAD synthesizing enzyme NMNAT2 in two siblings with childhood onset polyneuropathy with erythromelalgia. No additional homozygotes for this rare allele, which leads to amino acid substitution T94M, were present among the unaffected relatives tested or in the 60,000 exomes of the ExAC database. For axons to survive, axonal NMNAT2 activity has to be maintained above a threshold level but the T94M mutation confers a partial loss of function both in the ability of NMNAT2 to support axon survival and in its enzymatic properties. Electrophysiological tests and histological analysis of sural nerve biopsies in the patients were consistent with loss of distal sensory and motor axons. Thus, it is likely that NMNAT2 mutation causes this pain and axon loss phenotype making this the first disorder associated with mutation of a key regulator of Wallerian-like axon degeneration in humans. This supports indications from numerous animal studies that the Wallerian degeneration pathway is important in human disease and raises important questions about which other human phenotypes could be linked to this gene.Entities:
Keywords: Erythromelalgia; NAD; NMNAT2; Polyneuropathy; Wallerian degeneration
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Year: 2019 PMID: 31132363 DOI: 10.1016/j.expneurol.2019.112958
Source DB: PubMed Journal: Exp Neurol ISSN: 0014-4886 Impact factor: 5.330