Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium

OBJECTIVES: It is essential to understand the molecular basis of ovarian cancer etiology and tumor development to provide more effective preventive and therapeutic approaches to reduce mortality. Particularly, the molecular targets and pathways involved in early malignant transformation are still no...

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Autores principales: Zhang, Lifang, Wang, Dan, Jiang, Wei, Edwards, Dale, Qiu, Weiliang, Barroilhet, Lisa M, Rho, Jung-hyun, Jin, Lianjin, Seethappan, Vanitha, Vitonis, Allison, Wang, Jianliu, Mok, Samuel C, Crum, Christopher, Cramer, Daniel W, Ye, Bin
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2903602/
https://www.ncbi.nlm.nih.gov/pubmed/20576130
http://dx.doi.org/10.1186/1477-7827-8-74
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author Zhang, Lifang
Wang, Dan
Jiang, Wei
Edwards, Dale
Qiu, Weiliang
Barroilhet, Lisa M
Rho, Jung-hyun
Jin, Lianjin
Seethappan, Vanitha
Vitonis, Allison
Wang, Jianliu
Mok, Samuel C
Crum, Christopher
Cramer, Daniel W
Ye, Bin
author_facet Zhang, Lifang
Wang, Dan
Jiang, Wei
Edwards, Dale
Qiu, Weiliang
Barroilhet, Lisa M
Rho, Jung-hyun
Jin, Lianjin
Seethappan, Vanitha
Vitonis, Allison
Wang, Jianliu
Mok, Samuel C
Crum, Christopher
Cramer, Daniel W
Ye, Bin
author_sort Zhang, Lifang
collection PubMed
description OBJECTIVES: It is essential to understand the molecular basis of ovarian cancer etiology and tumor development to provide more effective preventive and therapeutic approaches to reduce mortality. Particularly, the molecular targets and pathways involved in early malignant transformation are still not clear. Pro-inflammatory lipids and pathways have been reported to play significant roles in ovarian cancer progression and metastasis. The major objective of this study was to explore and determine whether platelet activating factor (PAF) and receptor associated networking pathways might significantly induce malignant potential in BRCA1-mutant at-risk epithelial cells. METHODS: BRCA1-mutant ovarian epithelial cell lines including (HOSE-636, HOSE-642), BRCA1-mutant ovarian cancer cell (UWB1.289), wild type normal ovarian epithelial cell (HOSE-E6E7) and cancerous cell line (OVCA429), and the non-malignant BRCA1-mutant distal fallopian tube (fimbria) tissue specimens were used in this study. Mutation analysis, kinase microarray, western blot, immune staining, co-immune precipitation, cell cycle, apoptosis, proliferation and bioinformatic pathway analysis were applied. RESULTS: We found that PAF, as a potent pro-inflammatory mediator, induced significant anti-apoptotic effect in BRCA1-mutant ovarian surface epithelial cells, but not in wild type HOSE cells. With kinase microarray technology and the specific immune approaches, we found that phosphor-STAT1 was activated by 100 nM PAF treatment only in BRCA1-mutant associated at-risk ovarian epithelial cells and ovarian cancer cells, but not in BRCA1-wild type normal (HOSE-E6E7) or malignant (OVCA429) ovarian epithelial cells. Co-immune precipitation revealed that elevated PAFR expression is associated with protein-protein interactions of PAFR-FAK and FAK-STAT1 in BRCA1-mutant ovarian epithelial cells, but not in the wild-type control cells. CONCLUSION: Previous studies showed that potent inflammatory lipid mediators such as PAF and its receptor (PAFR) significantly contribute to cancer progression and metastasis. Our findings suggest that these potent inflammatory lipids and receptor pathways are significantly involved in the early malignant transformation through PAFR-FAK-STAT1 networking and to block apoptosis pathway in BRCA1 dysfunctional at-risk ovarian epithelium.
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spelling pubmed-29036022010-07-14 Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium Zhang, Lifang Wang, Dan Jiang, Wei Edwards, Dale Qiu, Weiliang Barroilhet, Lisa M Rho, Jung-hyun Jin, Lianjin Seethappan, Vanitha Vitonis, Allison Wang, Jianliu Mok, Samuel C Crum, Christopher Cramer, Daniel W Ye, Bin Reprod Biol Endocrinol Research OBJECTIVES: It is essential to understand the molecular basis of ovarian cancer etiology and tumor development to provide more effective preventive and therapeutic approaches to reduce mortality. Particularly, the molecular targets and pathways involved in early malignant transformation are still not clear. Pro-inflammatory lipids and pathways have been reported to play significant roles in ovarian cancer progression and metastasis. The major objective of this study was to explore and determine whether platelet activating factor (PAF) and receptor associated networking pathways might significantly induce malignant potential in BRCA1-mutant at-risk epithelial cells. METHODS: BRCA1-mutant ovarian epithelial cell lines including (HOSE-636, HOSE-642), BRCA1-mutant ovarian cancer cell (UWB1.289), wild type normal ovarian epithelial cell (HOSE-E6E7) and cancerous cell line (OVCA429), and the non-malignant BRCA1-mutant distal fallopian tube (fimbria) tissue specimens were used in this study. Mutation analysis, kinase microarray, western blot, immune staining, co-immune precipitation, cell cycle, apoptosis, proliferation and bioinformatic pathway analysis were applied. RESULTS: We found that PAF, as a potent pro-inflammatory mediator, induced significant anti-apoptotic effect in BRCA1-mutant ovarian surface epithelial cells, but not in wild type HOSE cells. With kinase microarray technology and the specific immune approaches, we found that phosphor-STAT1 was activated by 100 nM PAF treatment only in BRCA1-mutant associated at-risk ovarian epithelial cells and ovarian cancer cells, but not in BRCA1-wild type normal (HOSE-E6E7) or malignant (OVCA429) ovarian epithelial cells. Co-immune precipitation revealed that elevated PAFR expression is associated with protein-protein interactions of PAFR-FAK and FAK-STAT1 in BRCA1-mutant ovarian epithelial cells, but not in the wild-type control cells. CONCLUSION: Previous studies showed that potent inflammatory lipid mediators such as PAF and its receptor (PAFR) significantly contribute to cancer progression and metastasis. Our findings suggest that these potent inflammatory lipids and receptor pathways are significantly involved in the early malignant transformation through PAFR-FAK-STAT1 networking and to block apoptosis pathway in BRCA1 dysfunctional at-risk ovarian epithelium. BioMed Central 2010-06-24 /pmc/articles/PMC2903602/ /pubmed/20576130 http://dx.doi.org/10.1186/1477-7827-8-74 Text en Copyright ©2010 Zhang et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Zhang, Lifang
Wang, Dan
Jiang, Wei
Edwards, Dale
Qiu, Weiliang
Barroilhet, Lisa M
Rho, Jung-hyun
Jin, Lianjin
Seethappan, Vanitha
Vitonis, Allison
Wang, Jianliu
Mok, Samuel C
Crum, Christopher
Cramer, Daniel W
Ye, Bin
Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title_full Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title_fullStr Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title_full_unstemmed Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title_short Activated networking of platelet activating factor receptor and FAK/STAT1 induces malignant potential in BRCA1-mutant at-risk ovarian epithelium
title_sort activated networking of platelet activating factor receptor and fak/stat1 induces malignant potential in brca1-mutant at-risk ovarian epithelium
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2903602/
https://www.ncbi.nlm.nih.gov/pubmed/20576130
http://dx.doi.org/10.1186/1477-7827-8-74
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