Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway

Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway

Lianzhi Cui,1,2 Yawei Zhao,1 Yue Pan,1 Xiao Zheng,1 Dan Shao,1 Yong Jia,3 Kan He,1 Kun Li,3 Li Chen1,3 1Department of Pharmacology, College of Basic Medical Sciences, Jilin University, Changchun, 2Clinical Laboratory, Jilin Cancer Hospital, Changchun, 3School of Nursing, Jilin University, Changchun...

Full description

Bibliographic Details
Main Authors: Cui LZ, Zhao YW, Pan Y, Zheng X, Shao D, Jia Y, He K, Li K, Chen L
Format: Article
Language:English
Published: Dove Medical Press 2017-12-01
Series:OncoTargets and Therapy
Subjects:
ovarian cancer
repopulation
chemotherapy
apoptosis
FAK
Online Access:https://www.dovepress.com/chemotherapy-induces-ovarian-cancer-cell-repopulation-through-the-casp-peer-reviewed-article-OTT
id doaj-693834d7736b486ba727f3c6e785fbb4
record_format Article
spelling doaj-693834d7736b486ba727f3c6e785fbb42020-11-24T21:49:58ZengDove Medical PressOncoTargets and Therapy1178-69302017-12-01Volume 105817582635914Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathwayCui LZZhao YWPan YZheng XShao DJia YHe KLi KChen LLianzhi Cui,1,2 Yawei Zhao,1 Yue Pan,1 Xiao Zheng,1 Dan Shao,1 Yong Jia,3 Kan He,1 Kun Li,3 Li Chen1,3 1Department of Pharmacology, College of Basic Medical Sciences, Jilin University, Changchun, 2Clinical Laboratory, Jilin Cancer Hospital, Changchun, 3School of Nursing, Jilin University, Changchun, China Abstract: Recurrence is one of the major causes of high mortality in ovarian cancer. However, the mechanism of ovarian cancer recurrence after chemotherapy has not been fully understood. In the present study, we investigated the effect of chemotherapy-induced tumor microenvironment on the proliferation of SKOV3 cells. We have shown that SKOV3 cells repopulated faster in the culture medium from apoptotic SKOV3 ovarian cancer cells after 24 h of etoposide phosphate (VP-16) treatment. We found that during apoptosis, cleaved caspase 3 could activate cytosolic calcium-independent phospholipase A2, which stimulated the release of arachidonic acid (AA) and triggered the production of prostaglandin E2 (PGE2). An increased level of phosphorylated focal adhesion kinase (FAK) subsequently facilitated the reproliferation of SKOV3 cells, and VP-16-induced repopulation effects were partially reversed by the FAK inhibitor PF562271. Furthermore, the plasma AA-to-PGE2 ratio and tumoral FAK expression of ovarian cancer patients after chemotherapy were significantly lower than those before chemotherapy. Taken together, our results indicate that chemotherapy-induced apoptotic cancer cells can produce PGE2-enriched microenvironment through caspase 3-mediated AA metabolic pathway, which could lead to the abnormal activation of FAK and eventually accelerate the repopulation of SKOV3 cells. Our study provides novel insight into a mechanism that may be utilized to prevent ovarian cancer recurrence in response to chemotherapy. Keywords: ovarian cancer, repopulation, chemotherapy, apoptosis, FAK https://www.dovepress.com/chemotherapy-induces-ovarian-cancer-cell-repopulation-through-the-casp-peer-reviewed-article-OTTovarian cancerrepopulationchemotherapyapoptosisFAK
collection DOAJ
language English
format Article
sources DOAJ
author Cui LZ
Zhao YW
Pan Y
Zheng X
Shao D
Jia Y
He K
Li K
Chen L
spellingShingle Cui LZ
Zhao YW
Pan Y
Zheng X
Shao D
Jia Y
He K
Li K
Chen L
Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
OncoTargets and Therapy
ovarian cancer
repopulation
chemotherapy
apoptosis
FAK
author_facet Cui LZ
Zhao YW
Pan Y
Zheng X
Shao D
Jia Y
He K
Li K
Chen L
author_sort Cui LZ
title Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
title_short Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
title_full Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
title_fullStr Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
title_full_unstemmed Chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
title_sort chemotherapy induces ovarian cancer cell repopulation through the caspase 3-mediated arachidonic acid metabolic pathway
publisher Dove Medical Press
series OncoTargets and Therapy
issn 1178-6930
publishDate 2017-12-01
description Lianzhi Cui,1,2 Yawei Zhao,1 Yue Pan,1 Xiao Zheng,1 Dan Shao,1 Yong Jia,3 Kan He,1 Kun Li,3 Li Chen1,3 1Department of Pharmacology, College of Basic Medical Sciences, Jilin University, Changchun, 2Clinical Laboratory, Jilin Cancer Hospital, Changchun, 3School of Nursing, Jilin University, Changchun, China Abstract: Recurrence is one of the major causes of high mortality in ovarian cancer. However, the mechanism of ovarian cancer recurrence after chemotherapy has not been fully understood. In the present study, we investigated the effect of chemotherapy-induced tumor microenvironment on the proliferation of SKOV3 cells. We have shown that SKOV3 cells repopulated faster in the culture medium from apoptotic SKOV3 ovarian cancer cells after 24 h of etoposide phosphate (VP-16) treatment. We found that during apoptosis, cleaved caspase 3 could activate cytosolic calcium-independent phospholipase A2, which stimulated the release of arachidonic acid (AA) and triggered the production of prostaglandin E2 (PGE2). An increased level of phosphorylated focal adhesion kinase (FAK) subsequently facilitated the reproliferation of SKOV3 cells, and VP-16-induced repopulation effects were partially reversed by the FAK inhibitor PF562271. Furthermore, the plasma AA-to-PGE2 ratio and tumoral FAK expression of ovarian cancer patients after chemotherapy were significantly lower than those before chemotherapy. Taken together, our results indicate that chemotherapy-induced apoptotic cancer cells can produce PGE2-enriched microenvironment through caspase 3-mediated AA metabolic pathway, which could lead to the abnormal activation of FAK and eventually accelerate the repopulation of SKOV3 cells. Our study provides novel insight into a mechanism that may be utilized to prevent ovarian cancer recurrence in response to chemotherapy. Keywords: ovarian cancer, repopulation, chemotherapy, apoptosis, FAK 
topic ovarian cancer
repopulation
chemotherapy
apoptosis
FAK
url https://www.dovepress.com/chemotherapy-induces-ovarian-cancer-cell-repopulation-through-the-casp-peer-reviewed-article-OTT
work_keys_str_mv AT cuilz chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT zhaoyw chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT pany chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT zhengx chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT shaod chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT jiay chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT hek chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT lik chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
AT chenl chemotherapyinducesovariancancercellrepopulationthroughthecaspase3mediatedarachidonicacidmetabolicpathway
_version_ 1725886075594866688

Similar Items