Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat

One of the primary factors contributing to boar taint is the level of androstenone in porcine adipose tissues. A majority of the studies performed to identify candidate biomarkers for the synthesis of androstenone in testis tissues follow a reductionist approach, identifying and studying the effect...

Descripción completa

Detalles Bibliográficos
Autores principales: Sahadevan, Sudeep, Gunawan, Asep, Tholen, Ernst, Große-Brinkhaus, Christine, Tesfaye, Dawit, Schellander, Karl, Hofmann-Apitius, Martin, Cinar, Mehmet Ulas, Uddin, Muhammad Jasim
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3948775/
https://www.ncbi.nlm.nih.gov/pubmed/24614349
http://dx.doi.org/10.1371/journal.pone.0091077
_version_ 1782306828285116416
author Sahadevan, Sudeep
Gunawan, Asep
Tholen, Ernst
Große-Brinkhaus, Christine
Tesfaye, Dawit
Schellander, Karl
Hofmann-Apitius, Martin
Cinar, Mehmet Ulas
Uddin, Muhammad Jasim
author_facet Sahadevan, Sudeep
Gunawan, Asep
Tholen, Ernst
Große-Brinkhaus, Christine
Tesfaye, Dawit
Schellander, Karl
Hofmann-Apitius, Martin
Cinar, Mehmet Ulas
Uddin, Muhammad Jasim
author_sort Sahadevan, Sudeep
collection PubMed
description One of the primary factors contributing to boar taint is the level of androstenone in porcine adipose tissues. A majority of the studies performed to identify candidate biomarkers for the synthesis of androstenone in testis tissues follow a reductionist approach, identifying and studying the effect of biomarkers individually. Although these studies provide detailed information on individual biomarkers, a global picture of changes in metabolic pathways that lead to the difference in androstenone synthesis is still missing. The aim of this work was to identify major pathways and interactions influencing steroid hormone synthesis and androstenone biosynthesis using an integrative approach to provide a bird’s eye view of the factors causing difference in steroidogenesis and androstenone biosynthesis. For this purpose, we followed an analysis procedure merging together gene expression data from boars with divergent levels of androstenone and pathway mapping and interaction network retrieved from KEGG database. The interaction networks were weighted with Pearson correlation coefficients calculated from gene expression data and significant interactions and enriched pathways were identified based on these networks. The results show that 1,023 interactions were significant for high and low androstenone animals and that a total of 92 pathways were enriched for significant interactions. Although published articles show that a number of these enriched pathways were activated as a result of downstream signaling of steroid hormones, we speculate that the significant interactions in pathways such as glutathione metabolism, sphingolipid metabolism, fatty acid metabolism and significant interactions in cAMP-PKA/PKC signaling might be the key factors determining the difference in steroidogenesis and androstenone biosynthesis between boars with divergent androstenone levels in our study. The results and assumptions presented in this study are from an in-silico analysis done at the gene expression level and further laboratory experiments at genomic, proteomic or metabolomic level are necessary to validate these findings.
format Online
Article
Text
id pubmed-3948775
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-39487752014-03-13 Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat Sahadevan, Sudeep Gunawan, Asep Tholen, Ernst Große-Brinkhaus, Christine Tesfaye, Dawit Schellander, Karl Hofmann-Apitius, Martin Cinar, Mehmet Ulas Uddin, Muhammad Jasim PLoS One Research Article One of the primary factors contributing to boar taint is the level of androstenone in porcine adipose tissues. A majority of the studies performed to identify candidate biomarkers for the synthesis of androstenone in testis tissues follow a reductionist approach, identifying and studying the effect of biomarkers individually. Although these studies provide detailed information on individual biomarkers, a global picture of changes in metabolic pathways that lead to the difference in androstenone synthesis is still missing. The aim of this work was to identify major pathways and interactions influencing steroid hormone synthesis and androstenone biosynthesis using an integrative approach to provide a bird’s eye view of the factors causing difference in steroidogenesis and androstenone biosynthesis. For this purpose, we followed an analysis procedure merging together gene expression data from boars with divergent levels of androstenone and pathway mapping and interaction network retrieved from KEGG database. The interaction networks were weighted with Pearson correlation coefficients calculated from gene expression data and significant interactions and enriched pathways were identified based on these networks. The results show that 1,023 interactions were significant for high and low androstenone animals and that a total of 92 pathways were enriched for significant interactions. Although published articles show that a number of these enriched pathways were activated as a result of downstream signaling of steroid hormones, we speculate that the significant interactions in pathways such as glutathione metabolism, sphingolipid metabolism, fatty acid metabolism and significant interactions in cAMP-PKA/PKC signaling might be the key factors determining the difference in steroidogenesis and androstenone biosynthesis between boars with divergent androstenone levels in our study. The results and assumptions presented in this study are from an in-silico analysis done at the gene expression level and further laboratory experiments at genomic, proteomic or metabolomic level are necessary to validate these findings. Public Library of Science 2014-03-10 /pmc/articles/PMC3948775/ /pubmed/24614349 http://dx.doi.org/10.1371/journal.pone.0091077 Text en © 2014 Sahadevan 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
Sahadevan, Sudeep
Gunawan, Asep
Tholen, Ernst
Große-Brinkhaus, Christine
Tesfaye, Dawit
Schellander, Karl
Hofmann-Apitius, Martin
Cinar, Mehmet Ulas
Uddin, Muhammad Jasim
Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title_full Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title_fullStr Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title_full_unstemmed Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title_short Pathway Based Analysis of Genes and Interactions Influencing Porcine Testis Samples from Boars with Divergent Androstenone Content in Back Fat
title_sort pathway based analysis of genes and interactions influencing porcine testis samples from boars with divergent androstenone content in back fat
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3948775/
https://www.ncbi.nlm.nih.gov/pubmed/24614349
http://dx.doi.org/10.1371/journal.pone.0091077
work_keys_str_mv AT sahadevansudeep pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT gunawanasep pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT tholenernst pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT großebrinkhauschristine pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT tesfayedawit pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT schellanderkarl pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT hofmannapitiusmartin pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT cinarmehmetulas pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat
AT uddinmuhammadjasim pathwaybasedanalysisofgenesandinteractionsinfluencingporcinetestissamplesfromboarswithdivergentandrostenonecontentinbackfat

Ejemplares similares