Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy

Alaskan Husky Encephalopathy (AHE) has been previously proposed as a mitochondrial encephalopathy based on neuropathological similarities with human Leigh Syndrome (LS). We studied 11 Alaskan Husky dogs with AHE, but found no abnormalities in respiratory chain enzyme activities in muscle and liver,...

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Autores principales: Vernau, Karen M., Runstadler, Jonathan A., Brown, Emily A., Cameron, Jessie M., Huson, Heather J., Higgins, Robert J., Ackerley, Cameron, Sturges, Beverly K., Dickinson, Peter J., Puschner, Birgit, Giulivi, Cecilia, Shelton, G. Diane, Robinson, Brian H., DiMauro, Salvatore, Bollen, Andrew W., Bannasch, Danika L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3587633/
https://www.ncbi.nlm.nih.gov/pubmed/23469184
http://dx.doi.org/10.1371/journal.pone.0057195
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author Vernau, Karen M.
Runstadler, Jonathan A.
Brown, Emily A.
Cameron, Jessie M.
Huson, Heather J.
Higgins, Robert J.
Ackerley, Cameron
Sturges, Beverly K.
Dickinson, Peter J.
Puschner, Birgit
Giulivi, Cecilia
Shelton, G. Diane
Robinson, Brian H.
DiMauro, Salvatore
Bollen, Andrew W.
Bannasch, Danika L.
author_facet Vernau, Karen M.
Runstadler, Jonathan A.
Brown, Emily A.
Cameron, Jessie M.
Huson, Heather J.
Higgins, Robert J.
Ackerley, Cameron
Sturges, Beverly K.
Dickinson, Peter J.
Puschner, Birgit
Giulivi, Cecilia
Shelton, G. Diane
Robinson, Brian H.
DiMauro, Salvatore
Bollen, Andrew W.
Bannasch, Danika L.
author_sort Vernau, Karen M.
collection PubMed
description Alaskan Husky Encephalopathy (AHE) has been previously proposed as a mitochondrial encephalopathy based on neuropathological similarities with human Leigh Syndrome (LS). We studied 11 Alaskan Husky dogs with AHE, but found no abnormalities in respiratory chain enzyme activities in muscle and liver, or mutations in mitochondrial or nuclear genes that cause LS in people. A genome wide association study was performed using eight of the affected dogs and 20 related but unaffected control AHs using the Illumina canine HD array. SLC19A3 was identified as a positional candidate gene. This gene controls the uptake of thiamine in the CNS via expression of the thiamine transporter protein THTR2. Dogs have two copies of this gene located within the candidate interval (SLC19A3.2 – 43.36–43.38 Mb and SLC19A3.1 – 43.411–43.419 Mb) on chromosome 25. Expression analysis in a normal dog revealed that one of the paralogs, SLC19A3.1, was expressed in the brain and spinal cord while the other was not. Subsequent exon sequencing of SLC19A3.1 revealed a 4bp insertion and SNP in the second exon that is predicted to result in a functional protein truncation of 279 amino acids (c.624 insTTGC, c.625 C>A). All dogs with AHE were homozygous for this mutation, 15/41 healthy AH control dogs were heterozygous carriers while 26/41 normal healthy AH dogs were wild type. Furthermore, this mutation was not detected in another 187 dogs of different breeds. These results suggest that this mutation in SLC19A3.1, encoding a thiamine transporter protein, plays a critical role in the pathogenesis of AHE.
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spelling pubmed-35876332013-03-06 Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy Vernau, Karen M. Runstadler, Jonathan A. Brown, Emily A. Cameron, Jessie M. Huson, Heather J. Higgins, Robert J. Ackerley, Cameron Sturges, Beverly K. Dickinson, Peter J. Puschner, Birgit Giulivi, Cecilia Shelton, G. Diane Robinson, Brian H. DiMauro, Salvatore Bollen, Andrew W. Bannasch, Danika L. PLoS One Research Article Alaskan Husky Encephalopathy (AHE) has been previously proposed as a mitochondrial encephalopathy based on neuropathological similarities with human Leigh Syndrome (LS). We studied 11 Alaskan Husky dogs with AHE, but found no abnormalities in respiratory chain enzyme activities in muscle and liver, or mutations in mitochondrial or nuclear genes that cause LS in people. A genome wide association study was performed using eight of the affected dogs and 20 related but unaffected control AHs using the Illumina canine HD array. SLC19A3 was identified as a positional candidate gene. This gene controls the uptake of thiamine in the CNS via expression of the thiamine transporter protein THTR2. Dogs have two copies of this gene located within the candidate interval (SLC19A3.2 – 43.36–43.38 Mb and SLC19A3.1 – 43.411–43.419 Mb) on chromosome 25. Expression analysis in a normal dog revealed that one of the paralogs, SLC19A3.1, was expressed in the brain and spinal cord while the other was not. Subsequent exon sequencing of SLC19A3.1 revealed a 4bp insertion and SNP in the second exon that is predicted to result in a functional protein truncation of 279 amino acids (c.624 insTTGC, c.625 C>A). All dogs with AHE were homozygous for this mutation, 15/41 healthy AH control dogs were heterozygous carriers while 26/41 normal healthy AH dogs were wild type. Furthermore, this mutation was not detected in another 187 dogs of different breeds. These results suggest that this mutation in SLC19A3.1, encoding a thiamine transporter protein, plays a critical role in the pathogenesis of AHE. Public Library of Science 2013-03-04 /pmc/articles/PMC3587633/ /pubmed/23469184 http://dx.doi.org/10.1371/journal.pone.0057195 Text en © 2013 Vernau et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Vernau, Karen M.
Runstadler, Jonathan A.
Brown, Emily A.
Cameron, Jessie M.
Huson, Heather J.
Higgins, Robert J.
Ackerley, Cameron
Sturges, Beverly K.
Dickinson, Peter J.
Puschner, Birgit
Giulivi, Cecilia
Shelton, G. Diane
Robinson, Brian H.
DiMauro, Salvatore
Bollen, Andrew W.
Bannasch, Danika L.
Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title_full Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title_fullStr Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title_full_unstemmed Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title_short Genome-Wide Association Analysis Identifies a Mutation in the Thiamine Transporter 2 (SLC19A3) Gene Associated with Alaskan Husky Encephalopathy
title_sort genome-wide association analysis identifies a mutation in the thiamine transporter 2 (slc19a3) gene associated with alaskan husky encephalopathy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3587633/
https://www.ncbi.nlm.nih.gov/pubmed/23469184
http://dx.doi.org/10.1371/journal.pone.0057195
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