An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction

BACKGROUND: The identity and spatial distribution of prostatic cell types has been determined in humans but not in dogs, even though aging- and prostate-related voiding disorders are common in both species and mechanistic factors, such as prostatic collagen accumulation, appear to be shared between...

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Autores principales: Ruetten, Hannah, Cole, Clara, Wehber, Marlyse, Wegner, Kyle A., Girardi, Nicholas M., Peterson, Nelson T., Scharpf, Brandon R., Romero, Michael F., Wood, Michael W., Colopy, Sara A., Bjorling, Dale E., Vezina, Chad M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7390344/
https://www.ncbi.nlm.nih.gov/pubmed/32726309
http://dx.doi.org/10.1371/journal.pone.0232564
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author Ruetten, Hannah
Cole, Clara
Wehber, Marlyse
Wegner, Kyle A.
Girardi, Nicholas M.
Peterson, Nelson T.
Scharpf, Brandon R.
Romero, Michael F.
Wood, Michael W.
Colopy, Sara A.
Bjorling, Dale E.
Vezina, Chad M.
author_facet Ruetten, Hannah
Cole, Clara
Wehber, Marlyse
Wegner, Kyle A.
Girardi, Nicholas M.
Peterson, Nelson T.
Scharpf, Brandon R.
Romero, Michael F.
Wood, Michael W.
Colopy, Sara A.
Bjorling, Dale E.
Vezina, Chad M.
author_sort Ruetten, Hannah
collection PubMed
description BACKGROUND: The identity and spatial distribution of prostatic cell types has been determined in humans but not in dogs, even though aging- and prostate-related voiding disorders are common in both species and mechanistic factors, such as prostatic collagen accumulation, appear to be shared between species. In this publication we characterize the regional distribution of prostatic cell types in the young intact dog to enable comparisons with human and mice and we examine how the cellular source of procollagen 1A1 changes with age in intact male dogs. METHODS: A multichotomous decision tree involving sequential immunohistochemical stains was validated for use in dog and used to identify specific prostatic cell types and determine their distribution in the capsule, peripheral, periurethral and urethral regions of the young intact canine prostate. Prostatic cells identified using this technique include perivascular smooth muscle cells, pericytes, endothelial cells, luminal, intermediate, and basal epithelial cells, neuroendocrine cells, myofibroblasts, fibroblasts, fibrocytes, and other hematolymphoid cells. To enhance rigor and transparency, all high resolution images (representative images shown in the figures and biological replicates) are available through the GUDMAP database at https://doi.org/10.25548/16-WMM4. RESULTS: The prostatic peripheral region harbors the largest proportion of epithelial cells. Aging does not change the density of hematolymphoid cells, fibroblasts, and myofibroblasts in the peripheral region or in the fibromuscular capsule, regions where we previously observed aging- and androgen-mediated increases in prostatic collagen abundance Instead, we observed aging-related changes the procollagen 1A1 positive prostatic cell identity from a myofibroblast to a fibroblast. CONCLUSIONS: Hematolymphoid cells and myofibroblasts are often identified as sources of collagen in tissues prone to aging-related fibrosis. We show that these are not the likely sources of pathological collagen synthesis in older intact male dogs. Instead, we identify an aging-related shift in the prostatic cell type producing procollagen 1A1 that will help direct development of cell type and prostate appropriate therapeutics for collagen accumulation.
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spelling pubmed-73903442020-08-05 An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction Ruetten, Hannah Cole, Clara Wehber, Marlyse Wegner, Kyle A. Girardi, Nicholas M. Peterson, Nelson T. Scharpf, Brandon R. Romero, Michael F. Wood, Michael W. Colopy, Sara A. Bjorling, Dale E. Vezina, Chad M. PLoS One Research Article BACKGROUND: The identity and spatial distribution of prostatic cell types has been determined in humans but not in dogs, even though aging- and prostate-related voiding disorders are common in both species and mechanistic factors, such as prostatic collagen accumulation, appear to be shared between species. In this publication we characterize the regional distribution of prostatic cell types in the young intact dog to enable comparisons with human and mice and we examine how the cellular source of procollagen 1A1 changes with age in intact male dogs. METHODS: A multichotomous decision tree involving sequential immunohistochemical stains was validated for use in dog and used to identify specific prostatic cell types and determine their distribution in the capsule, peripheral, periurethral and urethral regions of the young intact canine prostate. Prostatic cells identified using this technique include perivascular smooth muscle cells, pericytes, endothelial cells, luminal, intermediate, and basal epithelial cells, neuroendocrine cells, myofibroblasts, fibroblasts, fibrocytes, and other hematolymphoid cells. To enhance rigor and transparency, all high resolution images (representative images shown in the figures and biological replicates) are available through the GUDMAP database at https://doi.org/10.25548/16-WMM4. RESULTS: The prostatic peripheral region harbors the largest proportion of epithelial cells. Aging does not change the density of hematolymphoid cells, fibroblasts, and myofibroblasts in the peripheral region or in the fibromuscular capsule, regions where we previously observed aging- and androgen-mediated increases in prostatic collagen abundance Instead, we observed aging-related changes the procollagen 1A1 positive prostatic cell identity from a myofibroblast to a fibroblast. CONCLUSIONS: Hematolymphoid cells and myofibroblasts are often identified as sources of collagen in tissues prone to aging-related fibrosis. We show that these are not the likely sources of pathological collagen synthesis in older intact male dogs. Instead, we identify an aging-related shift in the prostatic cell type producing procollagen 1A1 that will help direct development of cell type and prostate appropriate therapeutics for collagen accumulation. Public Library of Science 2020-07-29 /pmc/articles/PMC7390344/ /pubmed/32726309 http://dx.doi.org/10.1371/journal.pone.0232564 Text en © 2020 Ruetten 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
Ruetten, Hannah
Cole, Clara
Wehber, Marlyse
Wegner, Kyle A.
Girardi, Nicholas M.
Peterson, Nelson T.
Scharpf, Brandon R.
Romero, Michael F.
Wood, Michael W.
Colopy, Sara A.
Bjorling, Dale E.
Vezina, Chad M.
An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title_full An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title_fullStr An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title_full_unstemmed An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title_short An immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1A1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
title_sort immunohistochemical prostate cell identification key indicates that aging shifts procollagen 1a1 production from myofibroblasts to fibroblasts in dogs prone to prostate-related urinary dysfunction
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7390344/
https://www.ncbi.nlm.nih.gov/pubmed/32726309
http://dx.doi.org/10.1371/journal.pone.0232564
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