Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer

I. Hung Shao; Tzu Hsuan Chang; Ying Hsu Chang; Yu Hsin Hsieh; Ting Wen Sheng; Li Jen Wang; Yu Hsuan Chien; Liang Kang Huang; Yuan Cheng Chu; Hung Cheng Kan; Po Hung Lin; Kai Jie Yu; Ming Li Hsieh; Cheng Keng Chuang; Chun Te Wu; Chin Hsuan Hsieh; See Tong Pang

doi:10.3892/ol.2024.14617

Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer

I. Hung Shao, Tzu Hsuan Chang, Ying Hsu Chang, Yu Hsin Hsieh, Ting Wen Sheng, Li Jen Wang, Yu Hsuan Chien, Liang Kang Huang, Yuan Cheng Chu, Hung Cheng Kan, Po Hung Lin, Kai Jie Yu, Ming Li Hsieh, Cheng Keng Chuang, Chun Te Wu, Chin Hsuan Hsieh^*, See Tong Pang^*

^*Corresponding author for this work

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

1 Scopus citations

Abstract

Prostate cancer (PCa) is the second most prevalent malignancy in men worldwide. The risk factors for PCa include obesity, age and family history. Increased visceral fat has been associated with high PCa risk, which has prompted previous researchers to investigate the influence of body composition and fat distribution on PCa prognosis. However, there is a lack of studies focusing on the mechanisms and interactions between periprostatic adipose tissue (PPAT) and PCa cells. The present study investigated the association between the composition of pelvic adipose tissue and PCa aggressiveness to understand the role played by this tissue in PCa progression. Moreover, PPAT-conditioned medium (CM) was prepared to assess the influence of the PPAT secretome on the patho-physiology of PCa. The present study included 50 patients with localized PCa who received robot-assisted radical prostatectomy. Medical records were collected, magnetic resonance imaging scans were analyzed and body compositions were calculated to identify the associations between adipose tissue volume and clinical PCa aggressiveness. In addition, CM was prepared from PPAT and perivesical adipose tissue (PVAT) collected from 25 patients during surgery, and its effects on the PCa cell lines C4-2 and LNCaP, and the prostate epithelial cell line PZ-HPV-7, were investigated using a cell proliferation assay and RNA sequencing (RNA-seq). The results revealed that the initial prostate-specific antigen level was significantly correlated with pelvic and periprostatic adipose tissue volumes. In addition, PPAT volume was significantly higher in patients with extracapsular tumor extension. PCa cell proliferation was significantly reduced when the cells were cultured in PPAT-CM compared with when they were cultured in control- and PVAT-CM. RNA-seq revealed that immune responses, and the cell death and apoptosis pathways were enriched in PPAT-CM-cultured cells indicating that the cytokines or other factors secreted from PPAT-CM induced PCa cell apoptosis. These findings revealed that the PPAT secretome may inhibit PCa cell proliferation by activating immune responses and promoting cancer cell apoptosis. This mechanism may act as a first-line defense during the early stages of PCa.

Original language	English
Article number	485
Pages (from-to)	485
Journal	Oncology Letters
Volume	28
Issue number	4
DOIs	https://doi.org/10.3892/ol.2024.14617
State	Published - 01 10 2024
Externally published	Yes

Bibliographical note

Keywords

Gene Set Enrichment Analysis
clinical
flow cytometry
magnetic resonance imaging
prostate cancer

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3892/ol.2024.14617

Cite this

Shao, I. H., Chang, T. H., Chang, Y. H., Hsieh, Y. H., Sheng, T. W., Wang, L. J., Chien, Y. H., Huang, L. K., Chu, Y. C., Kan, H. C., Lin, P. H., Yu, K. J., Hsieh, M. L., Chuang, C. K., Wu, C. T., Hsieh, C. H., & Pang, S. T. (2024). Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer. Oncology Letters, 28(4), 485. Article 485. https://doi.org/10.3892/ol.2024.14617

@article{18199a0027cb424eb8150c0878c11b64,

title = "Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer",

abstract = "Prostate cancer (PCa) is the second most prevalent malignancy in men worldwide. The risk factors for PCa include obesity, age and family history. Increased visceral fat has been associated with high PCa risk, which has prompted previous researchers to investigate the influence of body composition and fat distribution on PCa prognosis. However, there is a lack of studies focusing on the mechanisms and interactions between periprostatic adipose tissue (PPAT) and PCa cells. The present study investigated the association between the composition of pelvic adipose tissue and PCa aggressiveness to understand the role played by this tissue in PCa progression. Moreover, PPAT-conditioned medium (CM) was prepared to assess the influence of the PPAT secretome on the patho-physiology of PCa. The present study included 50 patients with localized PCa who received robot-assisted radical prostatectomy. Medical records were collected, magnetic resonance imaging scans were analyzed and body compositions were calculated to identify the associations between adipose tissue volume and clinical PCa aggressiveness. In addition, CM was prepared from PPAT and perivesical adipose tissue (PVAT) collected from 25 patients during surgery, and its effects on the PCa cell lines C4-2 and LNCaP, and the prostate epithelial cell line PZ-HPV-7, were investigated using a cell proliferation assay and RNA sequencing (RNA-seq). The results revealed that the initial prostate-specific antigen level was significantly correlated with pelvic and periprostatic adipose tissue volumes. In addition, PPAT volume was significantly higher in patients with extracapsular tumor extension. PCa cell proliferation was significantly reduced when the cells were cultured in PPAT-CM compared with when they were cultured in control- and PVAT-CM. RNA-seq revealed that immune responses, and the cell death and apoptosis pathways were enriched in PPAT-CM-cultured cells indicating that the cytokines or other factors secreted from PPAT-CM induced PCa cell apoptosis. These findings revealed that the PPAT secretome may inhibit PCa cell proliferation by activating immune responses and promoting cancer cell apoptosis. This mechanism may act as a first-line defense during the early stages of PCa.",

keywords = "Gene Set Enrichment Analysis, clinical, flow cytometry, magnetic resonance imaging, prostate cancer",

author = "Shao, {I. Hung} and Chang, {Tzu Hsuan} and Chang, {Ying Hsu} and Hsieh, {Yu Hsin} and Sheng, {Ting Wen} and Wang, {Li Jen} and Chien, {Yu Hsuan} and Huang, {Liang Kang} and Chu, {Yuan Cheng} and Kan, {Hung Cheng} and Lin, {Po Hung} and Yu, {Kai Jie} and Hsieh, {Ming Li} and Chuang, {Cheng Keng} and Wu, {Chun Te} and Hsieh, {Chin Hsuan} and Pang, {See Tong}",

note = "Copyright: {\textcopyright} 2024 Shao et al.",

year = "2024",

month = oct,

day = "1",

doi = "10.3892/ol.2024.14617",

language = "英语",

volume = "28",

pages = "485",

journal = "Oncology Letters",

issn = "1792-1074",

publisher = "Spandidos Publications",

number = "4",

}

Shao, IH, Chang, TH, Chang, YH, Hsieh, YH, Sheng, TW, Wang, LJ, Chien, YH, Huang, LK, Chu, YC, Kan, HC, Lin, PH, Yu, KJ, Hsieh, ML, Chuang, CK, Wu, CT, Hsieh, CH & Pang, ST 2024, 'Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer', Oncology Letters, vol. 28, no. 4, 485, pp. 485. https://doi.org/10.3892/ol.2024.14617

Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer. / Shao, I. Hung; Chang, Tzu Hsuan; Chang, Ying Hsu et al.
In: Oncology Letters, Vol. 28, No. 4, 485, 01.10.2024, p. 485.

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

TY - JOUR

T1 - Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors

T2 - A natural barrier induced by the immune response during the early stages of prostate cancer

AU - Shao, I. Hung

AU - Chang, Tzu Hsuan

AU - Chang, Ying Hsu

AU - Hsieh, Yu Hsin

AU - Sheng, Ting Wen

AU - Wang, Li Jen

AU - Chien, Yu Hsuan

AU - Huang, Liang Kang

AU - Chu, Yuan Cheng

AU - Kan, Hung Cheng

AU - Lin, Po Hung

AU - Yu, Kai Jie

AU - Hsieh, Ming Li

AU - Chuang, Cheng Keng

AU - Wu, Chun Te

AU - Hsieh, Chin Hsuan

AU - Pang, See Tong

PY - 2024/10/1

Y1 - 2024/10/1

N2 - Prostate cancer (PCa) is the second most prevalent malignancy in men worldwide. The risk factors for PCa include obesity, age and family history. Increased visceral fat has been associated with high PCa risk, which has prompted previous researchers to investigate the influence of body composition and fat distribution on PCa prognosis. However, there is a lack of studies focusing on the mechanisms and interactions between periprostatic adipose tissue (PPAT) and PCa cells. The present study investigated the association between the composition of pelvic adipose tissue and PCa aggressiveness to understand the role played by this tissue in PCa progression. Moreover, PPAT-conditioned medium (CM) was prepared to assess the influence of the PPAT secretome on the patho-physiology of PCa. The present study included 50 patients with localized PCa who received robot-assisted radical prostatectomy. Medical records were collected, magnetic resonance imaging scans were analyzed and body compositions were calculated to identify the associations between adipose tissue volume and clinical PCa aggressiveness. In addition, CM was prepared from PPAT and perivesical adipose tissue (PVAT) collected from 25 patients during surgery, and its effects on the PCa cell lines C4-2 and LNCaP, and the prostate epithelial cell line PZ-HPV-7, were investigated using a cell proliferation assay and RNA sequencing (RNA-seq). The results revealed that the initial prostate-specific antigen level was significantly correlated with pelvic and periprostatic adipose tissue volumes. In addition, PPAT volume was significantly higher in patients with extracapsular tumor extension. PCa cell proliferation was significantly reduced when the cells were cultured in PPAT-CM compared with when they were cultured in control- and PVAT-CM. RNA-seq revealed that immune responses, and the cell death and apoptosis pathways were enriched in PPAT-CM-cultured cells indicating that the cytokines or other factors secreted from PPAT-CM induced PCa cell apoptosis. These findings revealed that the PPAT secretome may inhibit PCa cell proliferation by activating immune responses and promoting cancer cell apoptosis. This mechanism may act as a first-line defense during the early stages of PCa.

AB - Prostate cancer (PCa) is the second most prevalent malignancy in men worldwide. The risk factors for PCa include obesity, age and family history. Increased visceral fat has been associated with high PCa risk, which has prompted previous researchers to investigate the influence of body composition and fat distribution on PCa prognosis. However, there is a lack of studies focusing on the mechanisms and interactions between periprostatic adipose tissue (PPAT) and PCa cells. The present study investigated the association between the composition of pelvic adipose tissue and PCa aggressiveness to understand the role played by this tissue in PCa progression. Moreover, PPAT-conditioned medium (CM) was prepared to assess the influence of the PPAT secretome on the patho-physiology of PCa. The present study included 50 patients with localized PCa who received robot-assisted radical prostatectomy. Medical records were collected, magnetic resonance imaging scans were analyzed and body compositions were calculated to identify the associations between adipose tissue volume and clinical PCa aggressiveness. In addition, CM was prepared from PPAT and perivesical adipose tissue (PVAT) collected from 25 patients during surgery, and its effects on the PCa cell lines C4-2 and LNCaP, and the prostate epithelial cell line PZ-HPV-7, were investigated using a cell proliferation assay and RNA sequencing (RNA-seq). The results revealed that the initial prostate-specific antigen level was significantly correlated with pelvic and periprostatic adipose tissue volumes. In addition, PPAT volume was significantly higher in patients with extracapsular tumor extension. PCa cell proliferation was significantly reduced when the cells were cultured in PPAT-CM compared with when they were cultured in control- and PVAT-CM. RNA-seq revealed that immune responses, and the cell death and apoptosis pathways were enriched in PPAT-CM-cultured cells indicating that the cytokines or other factors secreted from PPAT-CM induced PCa cell apoptosis. These findings revealed that the PPAT secretome may inhibit PCa cell proliferation by activating immune responses and promoting cancer cell apoptosis. This mechanism may act as a first-line defense during the early stages of PCa.

KW - Gene Set Enrichment Analysis

KW - clinical

KW - flow cytometry

KW - magnetic resonance imaging

KW - prostate cancer

UR - http://www.scopus.com/inward/record.url?scp=85201446966&partnerID=8YFLogxK

U2 - 10.3892/ol.2024.14617

DO - 10.3892/ol.2024.14617

M3 - 文章

C2 - 39170882

AN - SCOPUS:85201446966

SN - 1792-1074

VL - 28

SP - 485

JO - Oncology Letters

JF - Oncology Letters

IS - 4

M1 - 485

ER -

Periprostatic adipose tissue inhibits tumor progression by secreting apoptotic factors: A natural barrier induced by the immune response during the early stages of prostate cancer

Abstract

Bibliographical note

Keywords

UN SDGs

Access to Document

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