The Expression of Inflammatory Mediators in Bladder Pain Syndrome

BACKGROUND: Bladder pain syndrome (BPS) pathology is poorly understood. Treatment strategies are empirical, with limited efficacy, and affected patients have diminished quality of life. OBJECTIVE: We examined the hypothesis that inflammatory mediators within the bladder contribute to BPS pathology....

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Autores principales: Offiah, Ifeoma, Didangelos, Athanasios, Dawes, John, Cartwright, Rufus, Khullar, Vik, Bradbury, Elizabeth J., O'Sullivan, Suzanne, Williams, Dic, Chessell, Iain P., Pallas, Kenny, Graham, Gerry, O’Reilly, Barry A., McMahon, Stephen B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier Science 2016
Materias:
Platinum Priority – Pelvic Pain
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4926725/
https://www.ncbi.nlm.nih.gov/pubmed/26965559
http://dx.doi.org/10.1016/j.eururo.2016.02.058
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author Offiah, Ifeoma
Didangelos, Athanasios
Dawes, John
Cartwright, Rufus
Khullar, Vik
Bradbury, Elizabeth J.
O'Sullivan, Suzanne
Williams, Dic
Chessell, Iain P.
Pallas, Kenny
Graham, Gerry
O’Reilly, Barry A.
McMahon, Stephen B.
author_facet Offiah, Ifeoma
Didangelos, Athanasios
Dawes, John
Cartwright, Rufus
Khullar, Vik
Bradbury, Elizabeth J.
O'Sullivan, Suzanne
Williams, Dic
Chessell, Iain P.
Pallas, Kenny
Graham, Gerry
O’Reilly, Barry A.
McMahon, Stephen B.
author_sort Offiah, Ifeoma
collection PubMed
description BACKGROUND: Bladder pain syndrome (BPS) pathology is poorly understood. Treatment strategies are empirical, with limited efficacy, and affected patients have diminished quality of life. OBJECTIVE: We examined the hypothesis that inflammatory mediators within the bladder contribute to BPS pathology. DESIGN, SETTING, AND PARTICIPANTS: Fifteen women with BPS and 15 women with stress urinary incontinence without bladder pain were recruited from Cork University Maternity Hospital from October 2011 to October 2012. During cystoscopy, 5-mm bladder biopsies were taken and processed for gene expression analysis. The effect of the identified genes was tested in laboratory animals. OUTCOME MEASURES AND STATISTICAL ANALYSIS: We studied the expression of 96 inflammation-related genes in diseased and healthy bladders. We measured the correlation between genes and patient clinical profiles using the Pearson correlation coefficient. RESULTS AND LIMITATIONS: Analysis revealed 15 differentially expressed genes, confirmed in a replication study. FGF7 and CCL21 correlated significantly with clinical outcomes. Intravesical CCL21 instillation in rats caused increased bladder excitability and increased c-fos activity in spinal cord neurons. CCL21 atypical receptor knockout mice showed significantly more c-fos upon bladder stimulation with CCL21 than wild-type littermates. There was no change in FGF7-treated animals. The variability in patient samples presented as the main limitation. We used principal component analysis to identify similarities within the patient group. CONCLUSIONS: Our study identified two biologically relevant inflammatory mediators in BPS and demonstrated an increase in nociceptive signalling with CCL21. Manipulation of this ligand is a potential new therapeutic strategy for BPS. PATIENT SUMMARY: We compared gene expression in bladder biopsies of patients with bladder pain syndrome (BPS) and controls without pain and identified two genes that were increased in BPS patients and correlated with clinical profiles. We tested the effect of these genes in laboratory animals, confirming their role in bladder pain. Manipulating these genes in BPS is a potential treatment strategy.
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spelling pubmed-49267252016-08-01 The Expression of Inflammatory Mediators in Bladder Pain Syndrome Offiah, Ifeoma Didangelos, Athanasios Dawes, John Cartwright, Rufus Khullar, Vik Bradbury, Elizabeth J. O'Sullivan, Suzanne Williams, Dic Chessell, Iain P. Pallas, Kenny Graham, Gerry O’Reilly, Barry A. McMahon, Stephen B. Eur Urol Platinum Priority – Pelvic Pain BACKGROUND: Bladder pain syndrome (BPS) pathology is poorly understood. Treatment strategies are empirical, with limited efficacy, and affected patients have diminished quality of life. OBJECTIVE: We examined the hypothesis that inflammatory mediators within the bladder contribute to BPS pathology. DESIGN, SETTING, AND PARTICIPANTS: Fifteen women with BPS and 15 women with stress urinary incontinence without bladder pain were recruited from Cork University Maternity Hospital from October 2011 to October 2012. During cystoscopy, 5-mm bladder biopsies were taken and processed for gene expression analysis. The effect of the identified genes was tested in laboratory animals. OUTCOME MEASURES AND STATISTICAL ANALYSIS: We studied the expression of 96 inflammation-related genes in diseased and healthy bladders. We measured the correlation between genes and patient clinical profiles using the Pearson correlation coefficient. RESULTS AND LIMITATIONS: Analysis revealed 15 differentially expressed genes, confirmed in a replication study. FGF7 and CCL21 correlated significantly with clinical outcomes. Intravesical CCL21 instillation in rats caused increased bladder excitability and increased c-fos activity in spinal cord neurons. CCL21 atypical receptor knockout mice showed significantly more c-fos upon bladder stimulation with CCL21 than wild-type littermates. There was no change in FGF7-treated animals. The variability in patient samples presented as the main limitation. We used principal component analysis to identify similarities within the patient group. CONCLUSIONS: Our study identified two biologically relevant inflammatory mediators in BPS and demonstrated an increase in nociceptive signalling with CCL21. Manipulation of this ligand is a potential new therapeutic strategy for BPS. PATIENT SUMMARY: We compared gene expression in bladder biopsies of patients with bladder pain syndrome (BPS) and controls without pain and identified two genes that were increased in BPS patients and correlated with clinical profiles. We tested the effect of these genes in laboratory animals, confirming their role in bladder pain. Manipulating these genes in BPS is a potential treatment strategy. Elsevier Science 2016-08 /pmc/articles/PMC4926725/ /pubmed/26965559 http://dx.doi.org/10.1016/j.eururo.2016.02.058 Text en © 2016 Elsevier B.V. on behalf of European Association of Urology. All rights reserved. http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Platinum Priority – Pelvic Pain
Offiah, Ifeoma
Didangelos, Athanasios
Dawes, John
Cartwright, Rufus
Khullar, Vik
Bradbury, Elizabeth J.
O'Sullivan, Suzanne
Williams, Dic
Chessell, Iain P.
Pallas, Kenny
Graham, Gerry
O’Reilly, Barry A.
McMahon, Stephen B.
The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title_full The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title_fullStr The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title_full_unstemmed The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title_short The Expression of Inflammatory Mediators in Bladder Pain Syndrome
title_sort expression of inflammatory mediators in bladder pain syndrome
topic Platinum Priority – Pelvic Pain
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4926725/
https://www.ncbi.nlm.nih.gov/pubmed/26965559
http://dx.doi.org/10.1016/j.eururo.2016.02.058
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