A human prostatic bacterial isolate alters the prostatic microenvironment and accelerates prostate cancer progression

Brian W. Simons; Nicholas M. Durham; Tullia C. Bruno; Joseph F. Grosso; Anthony J. Schaeffer; Ashley E. Ross; Paula J. Hurley; David M. Berman; Charles G. Drake; Praveen Thumbikat; Edward M. Schaeffer

doi:10.1002/path.4472

A human prostatic bacterial isolate alters the prostatic microenvironment and accelerates prostate cancer progression

Brian W. Simons, Nicholas M. Durham, Tullia C. Bruno, Joseph F. Grosso, Anthony J. Schaeffer, Ashley E. Ross, Paula J. Hurley, David M. Berman, Charles G. Drake, Praveen Thumbikat, Edward M. Schaeffer

School of Medicine

Research output: Contribution to journal › Article › peer-review

42 Scopus citations

Abstract

Inflammation is associated with several diseases of the prostate including benign enlargement and cancer, but a causal relationship has not been established. Our objective was to characterize the prostate inflammatory microenvironment after infection with a human prostate-derived bacterial strain and to determine the effect of inflammation on prostate cancer progression. To this end, we mimicked typical human prostate infection with retrograde urethral instillation of CP1, a human prostatic isolate of Escherichia coli. CP1 bacteria were tropic for the accessory sex glands and induced acute inflammation in the prostate and seminal vesicles, with chronic inflammation lasting at least 1 year. Compared to controls, infection induced both acute and chronic inflammation with epithelial hyperplasia, stromal hyperplasia, and inflammatory cell infiltrates. In areas of inflammation, epithelial proliferation and hyperplasia often persist, despite decreased expression of androgen receptor (AR). Inflammatory cells in the prostates of CP1-infected mice were characterized at 8 weeks post-infection by flow cytometry, which showed an increase in macrophages and lymphocytes, particularly Th17 cells. Inflammation was additionally assessed in the context of carcinogenesis. Multiplex cytokine profiles of inflamed prostates showed that distinct inflammatory cytokines were expressed during prostate inflammation and cancer, with a subset of cytokines synergistically increased during concurrent inflammation and cancer. Furthermore, CP1 infection in the Hi-Myc mouse model of prostate cancer accelerated the development of invasive prostate adenocarcinoma, with 70% more mice developing cancer by 4.5months of age. This study provides direct evidence that prostate inflammation accelerates prostate cancer progression and gives insight into the microenvironment changes induced by inflammation that may accelerate tumour initiation or progression.

Original language	English (US)
Pages (from-to)	478-489
Number of pages	12
Journal	Journal of Pathology
Volume	235
Issue number	3
DOIs	https://doi.org/10.1002/path.4472
State	Published - Feb 1 2015

Keywords

Escherichia coli
Inflammation
Mouse
Prostate
Prostatitis

ASJC Scopus subject areas

Pathology and Forensic Medicine

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10.1002/path.4472

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title = "A human prostatic bacterial isolate alters the prostatic microenvironment and accelerates prostate cancer progression",

abstract = "Inflammation is associated with several diseases of the prostate including benign enlargement and cancer, but a causal relationship has not been established. Our objective was to characterize the prostate inflammatory microenvironment after infection with a human prostate-derived bacterial strain and to determine the effect of inflammation on prostate cancer progression. To this end, we mimicked typical human prostate infection with retrograde urethral instillation of CP1, a human prostatic isolate of Escherichia coli. CP1 bacteria were tropic for the accessory sex glands and induced acute inflammation in the prostate and seminal vesicles, with chronic inflammation lasting at least 1 year. Compared to controls, infection induced both acute and chronic inflammation with epithelial hyperplasia, stromal hyperplasia, and inflammatory cell infiltrates. In areas of inflammation, epithelial proliferation and hyperplasia often persist, despite decreased expression of androgen receptor (AR). Inflammatory cells in the prostates of CP1-infected mice were characterized at 8 weeks post-infection by flow cytometry, which showed an increase in macrophages and lymphocytes, particularly Th17 cells. Inflammation was additionally assessed in the context of carcinogenesis. Multiplex cytokine profiles of inflamed prostates showed that distinct inflammatory cytokines were expressed during prostate inflammation and cancer, with a subset of cytokines synergistically increased during concurrent inflammation and cancer. Furthermore, CP1 infection in the Hi-Myc mouse model of prostate cancer accelerated the development of invasive prostate adenocarcinoma, with 70% more mice developing cancer by 4.5months of age. This study provides direct evidence that prostate inflammation accelerates prostate cancer progression and gives insight into the microenvironment changes induced by inflammation that may accelerate tumour initiation or progression.",

keywords = "Escherichia coli, Inflammation, Mouse, Prostate, Prostatitis",

author = "Simons, {Brian W.} and Durham, {Nicholas M.} and Bruno, {Tullia C.} and Grosso, {Joseph F.} and Schaeffer, {Anthony J.} and Ross, {Ashley E.} and Hurley, {Paula J.} and Berman, {David M.} and Drake, {Charles G.} and Praveen Thumbikat and Schaeffer, {Edward M.}",

note = "Publisher Copyright: {\textcopyright} 2014 Pathological Society of Great Britain and Ireland.",

year = "2015",

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doi = "10.1002/path.4472",

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T1 - A human prostatic bacterial isolate alters the prostatic microenvironment and accelerates prostate cancer progression

AU - Simons, Brian W.

AU - Durham, Nicholas M.

AU - Bruno, Tullia C.

AU - Grosso, Joseph F.

AU - Schaeffer, Anthony J.

AU - Ross, Ashley E.

AU - Hurley, Paula J.

AU - Berman, David M.

AU - Drake, Charles G.

AU - Thumbikat, Praveen

AU - Schaeffer, Edward M.

PY - 2015/2/1

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N2 - Inflammation is associated with several diseases of the prostate including benign enlargement and cancer, but a causal relationship has not been established. Our objective was to characterize the prostate inflammatory microenvironment after infection with a human prostate-derived bacterial strain and to determine the effect of inflammation on prostate cancer progression. To this end, we mimicked typical human prostate infection with retrograde urethral instillation of CP1, a human prostatic isolate of Escherichia coli. CP1 bacteria were tropic for the accessory sex glands and induced acute inflammation in the prostate and seminal vesicles, with chronic inflammation lasting at least 1 year. Compared to controls, infection induced both acute and chronic inflammation with epithelial hyperplasia, stromal hyperplasia, and inflammatory cell infiltrates. In areas of inflammation, epithelial proliferation and hyperplasia often persist, despite decreased expression of androgen receptor (AR). Inflammatory cells in the prostates of CP1-infected mice were characterized at 8 weeks post-infection by flow cytometry, which showed an increase in macrophages and lymphocytes, particularly Th17 cells. Inflammation was additionally assessed in the context of carcinogenesis. Multiplex cytokine profiles of inflamed prostates showed that distinct inflammatory cytokines were expressed during prostate inflammation and cancer, with a subset of cytokines synergistically increased during concurrent inflammation and cancer. Furthermore, CP1 infection in the Hi-Myc mouse model of prostate cancer accelerated the development of invasive prostate adenocarcinoma, with 70% more mice developing cancer by 4.5months of age. This study provides direct evidence that prostate inflammation accelerates prostate cancer progression and gives insight into the microenvironment changes induced by inflammation that may accelerate tumour initiation or progression.

AB - Inflammation is associated with several diseases of the prostate including benign enlargement and cancer, but a causal relationship has not been established. Our objective was to characterize the prostate inflammatory microenvironment after infection with a human prostate-derived bacterial strain and to determine the effect of inflammation on prostate cancer progression. To this end, we mimicked typical human prostate infection with retrograde urethral instillation of CP1, a human prostatic isolate of Escherichia coli. CP1 bacteria were tropic for the accessory sex glands and induced acute inflammation in the prostate and seminal vesicles, with chronic inflammation lasting at least 1 year. Compared to controls, infection induced both acute and chronic inflammation with epithelial hyperplasia, stromal hyperplasia, and inflammatory cell infiltrates. In areas of inflammation, epithelial proliferation and hyperplasia often persist, despite decreased expression of androgen receptor (AR). Inflammatory cells in the prostates of CP1-infected mice were characterized at 8 weeks post-infection by flow cytometry, which showed an increase in macrophages and lymphocytes, particularly Th17 cells. Inflammation was additionally assessed in the context of carcinogenesis. Multiplex cytokine profiles of inflamed prostates showed that distinct inflammatory cytokines were expressed during prostate inflammation and cancer, with a subset of cytokines synergistically increased during concurrent inflammation and cancer. Furthermore, CP1 infection in the Hi-Myc mouse model of prostate cancer accelerated the development of invasive prostate adenocarcinoma, with 70% more mice developing cancer by 4.5months of age. This study provides direct evidence that prostate inflammation accelerates prostate cancer progression and gives insight into the microenvironment changes induced by inflammation that may accelerate tumour initiation or progression.

KW - Escherichia coli

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KW - Prostatitis

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A human prostatic bacterial isolate alters the prostatic microenvironment and accelerates prostate cancer progression

Abstract

Keywords

ASJC Scopus subject areas

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