Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.

Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.

GNE myopathy (GNEM), also known as hereditary inclusion body myopathy (HIBM), is a late- onset, progressive myopathy caused by mutations in the GNE gene encoding the enzyme responsible for the first regulated step in the biosynthesis of sialic acid (SA). The disease is characterized by distal muscle...

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Main Authors: Yiumo Michael Chan, Paul Lee, Steve Jungles, Gabrielle Morris, Jaclyn Cadaoas, Alison Skrinar, Michel Vellard, Emil Kakkis
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5340369?pdf=render
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spelling doaj-3bffbb97bdd540608213ca1bf464019d2020-11-24T21:35:15ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01123e017326110.1371/journal.pone.0173261Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.Yiumo Michael ChanPaul LeeSteve JunglesGabrielle MorrisJaclyn CadaoasAlison SkrinarMichel VellardEmil KakkisGNE myopathy (GNEM), also known as hereditary inclusion body myopathy (HIBM), is a late- onset, progressive myopathy caused by mutations in the GNE gene encoding the enzyme responsible for the first regulated step in the biosynthesis of sialic acid (SA). The disease is characterized by distal muscle weakness in both the lower and upper extremities, with the quadriceps muscle relatively spared until the late stages of disease. To explore the role of SA synthesis in the disease, we conducted a comprehensive and systematic analysis of both free and total SA levels in a large cohort of GNEM patients and a mouse model. A sensitive LC/MS/MS assay was developed to quantify SA in serum and muscle homogenates. Mean serum free SA level was 0.166 μg/mL in patients and 18% lower (p<0.001) than that of age-matched control samples (0.203 μg/mL). In biopsies obtained from patients, mean free SA levels of different muscles ranged from 0.046-0.075 μg/μmol Cr and were markedly lower by 72-85% (p<0.001) than free SA from normal controls. Free SA was shown to constitute a small fraction (3-7%) of the total SA pool in muscle tissue. Differences in mean total SA levels in muscle from patients compared with normal controls were less distinct and more variable between different muscles, suggesting a small subset of sialylation targets could be responsible for the pathogenesis of GNEM. Normal quadriceps had significantly lower levels of free SA (reduced by 39%) and total SA (reduced by 53%) compared to normal gastrocnemius. A lower SA requirement for quadriceps may be linked to the reported quadriceps sparing in GNEM. Analysis of SA levels in GneM743T/M743T mutant mice corroborated the human study results. These results show that serum and muscle free SA is severely reduced in GNEM, which is consistent with the biochemical defect in SA synthesis associated with GNE mutations. These results therefore support the approach of reversing SA depletion as a potential treatment for GNEM patients.http://europepmc.org/articles/PMC5340369?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yiumo Michael Chan
Paul Lee
Steve Jungles
Gabrielle Morris
Jaclyn Cadaoas
Alison Skrinar
Michel Vellard
Emil Kakkis
spellingShingle Yiumo Michael Chan
Paul Lee
Steve Jungles
Gabrielle Morris
Jaclyn Cadaoas
Alison Skrinar
Michel Vellard
Emil Kakkis
Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
PLoS ONE
author_facet Yiumo Michael Chan
Paul Lee
Steve Jungles
Gabrielle Morris
Jaclyn Cadaoas
Alison Skrinar
Michel Vellard
Emil Kakkis
author_sort Yiumo Michael Chan
title Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
title_short Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
title_full Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
title_fullStr Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
title_full_unstemmed Substantial deficiency of free sialic acid in muscles of patients with GNE myopathy and in a mouse model.
title_sort substantial deficiency of free sialic acid in muscles of patients with gne myopathy and in a mouse model.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description GNE myopathy (GNEM), also known as hereditary inclusion body myopathy (HIBM), is a late- onset, progressive myopathy caused by mutations in the GNE gene encoding the enzyme responsible for the first regulated step in the biosynthesis of sialic acid (SA). The disease is characterized by distal muscle weakness in both the lower and upper extremities, with the quadriceps muscle relatively spared until the late stages of disease. To explore the role of SA synthesis in the disease, we conducted a comprehensive and systematic analysis of both free and total SA levels in a large cohort of GNEM patients and a mouse model. A sensitive LC/MS/MS assay was developed to quantify SA in serum and muscle homogenates. Mean serum free SA level was 0.166 μg/mL in patients and 18% lower (p<0.001) than that of age-matched control samples (0.203 μg/mL). In biopsies obtained from patients, mean free SA levels of different muscles ranged from 0.046-0.075 μg/μmol Cr and were markedly lower by 72-85% (p<0.001) than free SA from normal controls. Free SA was shown to constitute a small fraction (3-7%) of the total SA pool in muscle tissue. Differences in mean total SA levels in muscle from patients compared with normal controls were less distinct and more variable between different muscles, suggesting a small subset of sialylation targets could be responsible for the pathogenesis of GNEM. Normal quadriceps had significantly lower levels of free SA (reduced by 39%) and total SA (reduced by 53%) compared to normal gastrocnemius. A lower SA requirement for quadriceps may be linked to the reported quadriceps sparing in GNEM. Analysis of SA levels in GneM743T/M743T mutant mice corroborated the human study results. These results show that serum and muscle free SA is severely reduced in GNEM, which is consistent with the biochemical defect in SA synthesis associated with GNE mutations. These results therefore support the approach of reversing SA depletion as a potential treatment for GNEM patients.
url http://europepmc.org/articles/PMC5340369?pdf=render
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