The G-protein coupled chemoattractant receptor FPR2 promotes malignant phenotype of human colon cancer cells

Yi Xiang; Xiaohong Yao; Keqiang Chen; Xiafei Wang; Jiamin Zhou; Wanghua Gong; Teizo Yoshimura; Jiaqiang Huang; Rongquan Wang; Yuzhang Wu; Guochao Shi; Xiuwu Bian; Jiming Wang

The G-protein coupled chemoattractant receptor FPR2 promotes malignant phenotype of human colon cancer cells

Yi Xiang, Xiaohong Yao, Keqiang Chen, Xiafei Wang, Jiamin Zhou, Wanghua Gong, Teizo Yoshimura, Jiaqiang Huang, Rongquan Wang, Yuzhang Wu, Guochao Shi, Xiuwu Bian, Jiming Wang

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

38 Citations (Scopus)

Abstract

The G-protein coupled chemoattractant receptor formylpeptide receptor-2 (FPR2 in human, Fpr2 in mice) is expressed by mouse colon epithelial cells and plays a critical role in mediating mucosal homeostasis and inflammatory responses. However, the biological role of FPR2 in human colon is unclear. Our investigation revealed that a considerable number of human colon cancer cell lines expressed FPR2 and its ligands promoted cell migration and proliferation. Human colon cancer cell lines expressing high levels of FPR2 also formed more rapidly growing tumors in immunocompromised mice as compared with cell lines expressing lower levels of FPR2. Knocking down of FPR2 from colon cancer cell lines highly expressing FPR2 reduced their tumorigenicity. Clinically, FPR2 is more highly expressed in progressive colon cancer, associated with poorer patient prognosis. These results suggest that FPR2 can be high-jacked by colon cancer cells for their growth advantage, thus becoming a potential target for therapeutic development.

Original language	English
Pages (from-to)	2599-2610
Number of pages	12
Journal	American Journal of Cancer Research
Volume	6
Issue number	11
Publication status	Published - 2016

Keywords

Cancer
Colon
FPR2
Prognosis
Tumorigenesis

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

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

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title = "The G-protein coupled chemoattractant receptor FPR2 promotes malignant phenotype of human colon cancer cells",

abstract = "The G-protein coupled chemoattractant receptor formylpeptide receptor-2 (FPR2 in human, Fpr2 in mice) is expressed by mouse colon epithelial cells and plays a critical role in mediating mucosal homeostasis and inflammatory responses. However, the biological role of FPR2 in human colon is unclear. Our investigation revealed that a considerable number of human colon cancer cell lines expressed FPR2 and its ligands promoted cell migration and proliferation. Human colon cancer cell lines expressing high levels of FPR2 also formed more rapidly growing tumors in immunocompromised mice as compared with cell lines expressing lower levels of FPR2. Knocking down of FPR2 from colon cancer cell lines highly expressing FPR2 reduced their tumorigenicity. Clinically, FPR2 is more highly expressed in progressive colon cancer, associated with poorer patient prognosis. These results suggest that FPR2 can be high-jacked by colon cancer cells for their growth advantage, thus becoming a potential target for therapeutic development.",

keywords = "Cancer, Colon, FPR2, Prognosis, Tumorigenesis",

author = "Yi Xiang and Xiaohong Yao and Keqiang Chen and Xiafei Wang and Jiamin Zhou and Wanghua Gong and Teizo Yoshimura and Jiaqiang Huang and Rongquan Wang and Yuzhang Wu and Guochao Shi and Xiuwu Bian and Jiming Wang",

note = "Funding Information: The authors thank Dr. A. Tominaga of the De-partment of Molecule and Cellular Biology, Kochi University, Kochi, Japan for providing FPCK-1-1, a normal human colon epithelial cell line; Dr. J. J. Oppenheim for critically reviewing the manuscript; Ms. C. Lamb and Ms. S. Livi-ngstone for secretarial assistance. This project was funded in part by federal funds from the National Cancer Institute, National Institutes of Health, under Contract No. HHSN261200800-001E and was supported in part by the Intramural Research Program of the NCI, NIH.",

year = "2016",

language = "English",

volume = "6",

pages = "2599--2610",

journal = "American Journal of Cancer Research",

issn = "2156-6976",

publisher = "e-Century Publishing Corporation",

number = "11",

}

TY - JOUR

T1 - The G-protein coupled chemoattractant receptor FPR2 promotes malignant phenotype of human colon cancer cells

AU - Xiang, Yi

AU - Yao, Xiaohong

AU - Chen, Keqiang

AU - Wang, Xiafei

AU - Zhou, Jiamin

AU - Gong, Wanghua

AU - Yoshimura, Teizo

AU - Huang, Jiaqiang

AU - Wang, Rongquan

AU - Wu, Yuzhang

AU - Shi, Guochao

AU - Bian, Xiuwu

AU - Wang, Jiming

N1 - Funding Information: The authors thank Dr. A. Tominaga of the De-partment of Molecule and Cellular Biology, Kochi University, Kochi, Japan for providing FPCK-1-1, a normal human colon epithelial cell line; Dr. J. J. Oppenheim for critically reviewing the manuscript; Ms. C. Lamb and Ms. S. Livi-ngstone for secretarial assistance. This project was funded in part by federal funds from the National Cancer Institute, National Institutes of Health, under Contract No. HHSN261200800-001E and was supported in part by the Intramural Research Program of the NCI, NIH.

PY - 2016

Y1 - 2016

N2 - The G-protein coupled chemoattractant receptor formylpeptide receptor-2 (FPR2 in human, Fpr2 in mice) is expressed by mouse colon epithelial cells and plays a critical role in mediating mucosal homeostasis and inflammatory responses. However, the biological role of FPR2 in human colon is unclear. Our investigation revealed that a considerable number of human colon cancer cell lines expressed FPR2 and its ligands promoted cell migration and proliferation. Human colon cancer cell lines expressing high levels of FPR2 also formed more rapidly growing tumors in immunocompromised mice as compared with cell lines expressing lower levels of FPR2. Knocking down of FPR2 from colon cancer cell lines highly expressing FPR2 reduced their tumorigenicity. Clinically, FPR2 is more highly expressed in progressive colon cancer, associated with poorer patient prognosis. These results suggest that FPR2 can be high-jacked by colon cancer cells for their growth advantage, thus becoming a potential target for therapeutic development.

AB - The G-protein coupled chemoattractant receptor formylpeptide receptor-2 (FPR2 in human, Fpr2 in mice) is expressed by mouse colon epithelial cells and plays a critical role in mediating mucosal homeostasis and inflammatory responses. However, the biological role of FPR2 in human colon is unclear. Our investigation revealed that a considerable number of human colon cancer cell lines expressed FPR2 and its ligands promoted cell migration and proliferation. Human colon cancer cell lines expressing high levels of FPR2 also formed more rapidly growing tumors in immunocompromised mice as compared with cell lines expressing lower levels of FPR2. Knocking down of FPR2 from colon cancer cell lines highly expressing FPR2 reduced their tumorigenicity. Clinically, FPR2 is more highly expressed in progressive colon cancer, associated with poorer patient prognosis. These results suggest that FPR2 can be high-jacked by colon cancer cells for their growth advantage, thus becoming a potential target for therapeutic development.

KW - Cancer

KW - Colon

KW - FPR2

KW - Prognosis

KW - Tumorigenesis

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SP - 2599

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JO - American Journal of Cancer Research

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ER -

The G-protein coupled chemoattractant receptor FPR2 promotes malignant phenotype of human colon cancer cells

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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