Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction

Disorders of sex development (DSD) and reproduction are not uncommon among horses, though knowledge about their molecular causes is sparse. Here we characterized a ~200 kb homozygous deletion in chromosome 29 at 29.7–29.9 Mb. The region contains AKR1C genes which function as ketosteroid reductases i...

Descripción completa

Detalles Bibliográficos
Autores principales: Ghosh, Sharmila, Davis, Brian W., Rosengren, Maria, Jevit, Matthew J., Castaneda, Caitlin, Arnold, Carolyn, Jaxheimer, Jay, Love, Charles C., Varner, Dickson D., Lindgren, Gabriella, Wade, Claire M., Raudsepp, Terje
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7140900/
https://www.ncbi.nlm.nih.gov/pubmed/32120906
http://dx.doi.org/10.3390/genes11030251
_version_ 1783519095077994496
author Ghosh, Sharmila
Davis, Brian W.
Rosengren, Maria
Jevit, Matthew J.
Castaneda, Caitlin
Arnold, Carolyn
Jaxheimer, Jay
Love, Charles C.
Varner, Dickson D.
Lindgren, Gabriella
Wade, Claire M.
Raudsepp, Terje
author_facet Ghosh, Sharmila
Davis, Brian W.
Rosengren, Maria
Jevit, Matthew J.
Castaneda, Caitlin
Arnold, Carolyn
Jaxheimer, Jay
Love, Charles C.
Varner, Dickson D.
Lindgren, Gabriella
Wade, Claire M.
Raudsepp, Terje
author_sort Ghosh, Sharmila
collection PubMed
description Disorders of sex development (DSD) and reproduction are not uncommon among horses, though knowledge about their molecular causes is sparse. Here we characterized a ~200 kb homozygous deletion in chromosome 29 at 29.7–29.9 Mb. The region contains AKR1C genes which function as ketosteroid reductases in steroid hormone biosynthesis, including androgens and estrogens. Mutations in AKR1C genes are associated with human DSDs. Deletion boundaries, sequence properties and gene content were studied by PCR and whole genome sequencing of select deletion homozygotes and control animals. Deletion analysis by PCR in 940 horses, including 622 with DSDs and reproductive problems and 318 phenotypically normal controls, detected 67 deletion homozygotes of which 79% were developmentally or reproductively abnormal. Altogether, 8–9% of all abnormal horses were homozygous for the deletion, with the highest incidence (9.4%) among cryptorchids. The deletion was found in ~4% of our phenotypically normal cohort, ~1% of global warmblood horses and ponies, and ~7% of draught breeds of general horse population as retrieved from published data. Based on the abnormal phenotype of the carriers, the functionally relevant gene content, and the low incidence in general population, we consider the deletion in chromosome 29 as a risk factor for equine DSDs and reproductive disorders.
format Online
Article
Text
id pubmed-7140900
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-71409002020-04-10 Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction Ghosh, Sharmila Davis, Brian W. Rosengren, Maria Jevit, Matthew J. Castaneda, Caitlin Arnold, Carolyn Jaxheimer, Jay Love, Charles C. Varner, Dickson D. Lindgren, Gabriella Wade, Claire M. Raudsepp, Terje Genes (Basel) Article Disorders of sex development (DSD) and reproduction are not uncommon among horses, though knowledge about their molecular causes is sparse. Here we characterized a ~200 kb homozygous deletion in chromosome 29 at 29.7–29.9 Mb. The region contains AKR1C genes which function as ketosteroid reductases in steroid hormone biosynthesis, including androgens and estrogens. Mutations in AKR1C genes are associated with human DSDs. Deletion boundaries, sequence properties and gene content were studied by PCR and whole genome sequencing of select deletion homozygotes and control animals. Deletion analysis by PCR in 940 horses, including 622 with DSDs and reproductive problems and 318 phenotypically normal controls, detected 67 deletion homozygotes of which 79% were developmentally or reproductively abnormal. Altogether, 8–9% of all abnormal horses were homozygous for the deletion, with the highest incidence (9.4%) among cryptorchids. The deletion was found in ~4% of our phenotypically normal cohort, ~1% of global warmblood horses and ponies, and ~7% of draught breeds of general horse population as retrieved from published data. Based on the abnormal phenotype of the carriers, the functionally relevant gene content, and the low incidence in general population, we consider the deletion in chromosome 29 as a risk factor for equine DSDs and reproductive disorders. MDPI 2020-02-27 /pmc/articles/PMC7140900/ /pubmed/32120906 http://dx.doi.org/10.3390/genes11030251 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ghosh, Sharmila
Davis, Brian W.
Rosengren, Maria
Jevit, Matthew J.
Castaneda, Caitlin
Arnold, Carolyn
Jaxheimer, Jay
Love, Charles C.
Varner, Dickson D.
Lindgren, Gabriella
Wade, Claire M.
Raudsepp, Terje
Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title_full Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title_fullStr Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title_full_unstemmed Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title_short Characterization of a Homozygous Deletion of Steroid Hormone Biosynthesis Genes in Horse Chromosome 29 as a Risk Factor for Disorders of Sex Development and Reproduction
title_sort characterization of a homozygous deletion of steroid hormone biosynthesis genes in horse chromosome 29 as a risk factor for disorders of sex development and reproduction
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7140900/
https://www.ncbi.nlm.nih.gov/pubmed/32120906
http://dx.doi.org/10.3390/genes11030251
work_keys_str_mv AT ghoshsharmila characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT davisbrianw characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT rosengrenmaria characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT jevitmatthewj characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT castanedacaitlin characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT arnoldcarolyn characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT jaxheimerjay characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT lovecharlesc characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT varnerdicksond characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT lindgrengabriella characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT wadeclairem characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction
AT raudseppterje characterizationofahomozygousdeletionofsteroidhormonebiosynthesisgenesinhorsechromosome29asariskfactorfordisordersofsexdevelopmentandreproduction

Ejemplares similares