RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis

Previous work demonstrates that the hearing loss in Alport mice is caused by defects in the stria vascularis. As the animals age, progressive thickening of strial capillary basement membranes (SCBMs) occurs associated with elevated levels of extracellular matrix expression and hypoxia-related gene a...

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Autores principales: Dufek, Brianna, Meehan, Daniel T., Delimont, Duane, Wilhelm, Kevin, Samuelson, Gina, Coenen, Ross, Madison, Jacob, Doyle, Edward, Smyth, Brendan, Phillips, Grady, Gratton, Michael Anne, Cosgrove, Dominic
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7446819/
https://www.ncbi.nlm.nih.gov/pubmed/32822386
http://dx.doi.org/10.1371/journal.pone.0237907
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author Dufek, Brianna
Meehan, Daniel T.
Delimont, Duane
Wilhelm, Kevin
Samuelson, Gina
Coenen, Ross
Madison, Jacob
Doyle, Edward
Smyth, Brendan
Phillips, Grady
Gratton, Michael Anne
Cosgrove, Dominic
author_facet Dufek, Brianna
Meehan, Daniel T.
Delimont, Duane
Wilhelm, Kevin
Samuelson, Gina
Coenen, Ross
Madison, Jacob
Doyle, Edward
Smyth, Brendan
Phillips, Grady
Gratton, Michael Anne
Cosgrove, Dominic
author_sort Dufek, Brianna
collection PubMed
description Previous work demonstrates that the hearing loss in Alport mice is caused by defects in the stria vascularis. As the animals age, progressive thickening of strial capillary basement membranes (SCBMs) occurs associated with elevated levels of extracellular matrix expression and hypoxia-related gene and protein expression. These conditions render the animals susceptible to noise-induced hearing loss. In an effort to develop a more comprehensive understanding of how the underlying mutation in the COL4A3 gene influences homeostasis in the stria vascularis, we performed vascular permeability studies combined with RNA-seq analysis using isolated stria vascularis from 7-week old wild-type and Alport mice on the 129 Sv background. Alport SCBMs were found to be less permeable than wild-type littermates. RNA-seq and bioinformatics analysis revealed 68 genes were induced and 61 genes suppressed in the stria from Alport mice relative to wild-type using a cut-off of 2-fold. These included pathways involving transcription factors associated with the regulation of pro-inflammatory responses as well as cytokines, chemokines, and chemokine receptors that are up- or down-regulated. Canonical pathways included modulation of genes associated with glucose and glucose-1-PO4 degradation, NAD biosynthesis, histidine degradation, calcium signaling, and glutamate receptor signaling (among others). In all, the data point to the Alport stria being in an inflammatory state with disruption in numerous metabolic pathways indicative of metabolic stress, a likely cause for the susceptibility of Alport mice to noise-induced hearing loss under conditions that do not cause permanent hearing loss in age/strain-matched wild-type mice. The work lays the foundation for studies aimed at understanding the nature of strial pathology in Alport mice. The modulation of these genes under conditions of therapeutic intervention may provide important pre-clinical data to justify trials in humans afflicted with the disease.
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spelling pubmed-74468192020-08-26 RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis Dufek, Brianna Meehan, Daniel T. Delimont, Duane Wilhelm, Kevin Samuelson, Gina Coenen, Ross Madison, Jacob Doyle, Edward Smyth, Brendan Phillips, Grady Gratton, Michael Anne Cosgrove, Dominic PLoS One Research Article Previous work demonstrates that the hearing loss in Alport mice is caused by defects in the stria vascularis. As the animals age, progressive thickening of strial capillary basement membranes (SCBMs) occurs associated with elevated levels of extracellular matrix expression and hypoxia-related gene and protein expression. These conditions render the animals susceptible to noise-induced hearing loss. In an effort to develop a more comprehensive understanding of how the underlying mutation in the COL4A3 gene influences homeostasis in the stria vascularis, we performed vascular permeability studies combined with RNA-seq analysis using isolated stria vascularis from 7-week old wild-type and Alport mice on the 129 Sv background. Alport SCBMs were found to be less permeable than wild-type littermates. RNA-seq and bioinformatics analysis revealed 68 genes were induced and 61 genes suppressed in the stria from Alport mice relative to wild-type using a cut-off of 2-fold. These included pathways involving transcription factors associated with the regulation of pro-inflammatory responses as well as cytokines, chemokines, and chemokine receptors that are up- or down-regulated. Canonical pathways included modulation of genes associated with glucose and glucose-1-PO4 degradation, NAD biosynthesis, histidine degradation, calcium signaling, and glutamate receptor signaling (among others). In all, the data point to the Alport stria being in an inflammatory state with disruption in numerous metabolic pathways indicative of metabolic stress, a likely cause for the susceptibility of Alport mice to noise-induced hearing loss under conditions that do not cause permanent hearing loss in age/strain-matched wild-type mice. The work lays the foundation for studies aimed at understanding the nature of strial pathology in Alport mice. The modulation of these genes under conditions of therapeutic intervention may provide important pre-clinical data to justify trials in humans afflicted with the disease. Public Library of Science 2020-08-21 /pmc/articles/PMC7446819/ /pubmed/32822386 http://dx.doi.org/10.1371/journal.pone.0237907 Text en © 2020 Dufek 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Dufek, Brianna
Meehan, Daniel T.
Delimont, Duane
Wilhelm, Kevin
Samuelson, Gina
Coenen, Ross
Madison, Jacob
Doyle, Edward
Smyth, Brendan
Phillips, Grady
Gratton, Michael Anne
Cosgrove, Dominic
RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title_full RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title_fullStr RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title_full_unstemmed RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title_short RNA-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and Alport mice reveals key pathways underling Alport strial pathogenesis
title_sort rna-seq analysis of gene expression profiles in isolated stria vascularis from wild-type and alport mice reveals key pathways underling alport strial pathogenesis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7446819/
https://www.ncbi.nlm.nih.gov/pubmed/32822386
http://dx.doi.org/10.1371/journal.pone.0237907
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