Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways

Qing-jun Liu,* Hong-liang Shen,* Jun Lin, Xiu-hong Xu, Zheng-guo Ji, Xiao Han, Dong-hao Shang, Pei-qian YangDepartment of Urology Surgery, Beijing Friendship Hospital, Capital Medical University, Beijing, People’s Republic of China*These authors contributed equally to this workInt...

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Main Authors: Liu QJ, Shen HL, Lin J, Xu XH, Ji ZG, Han X, Shang DH, Yang PQ
Format: Article
Language:English
Published: Dove Medical Press 2016-02-01
Series:Drug Design, Development and Therapy
Subjects:
p53
Online Access:https://www.dovepress.com/synergistic-roles-of-p53-and-hif1alpha-in-human-renal-cell-carcinoma-c-peer-reviewed-article-DDDT
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spelling doaj-b9dbd2c438694e2f93ecb5477f6f88752020-11-25T00:28:57ZengDove Medical PressDrug Design, Development and Therapy1177-88812016-02-012016Issue 174575525642Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathwaysLiu QJShen HLLin JXu XHJi ZGHan XShang DHYang PQQing-jun Liu,* Hong-liang Shen,* Jun Lin, Xiu-hong Xu, Zheng-guo Ji, Xiao Han, Dong-hao Shang, Pei-qian YangDepartment of Urology Surgery, Beijing Friendship Hospital, Capital Medical University, Beijing, People’s Republic of China*These authors contributed equally to this workIntroduction: mTOR and MDM2 signaling pathways are frequently deregulated in cancer development, and inhibition of mTOR or MDM2 independently enhances carcinoma-cell apoptosis. However, responses to mTOR and MDM2 antagonists in renal cell carcinoma (RCC) remain unknown.Materials and methods: A498 cells treated with MDM2 antagonist MI-319 and/or mTOR inhibitor rapamycin were employed in the present study. Cell apoptosis and Western blot analysis were performed.Results and conclusion: We found that the MDM2 inhibitor MI-319 induced RCC cell apoptosis mainly dependent on p53 overexpression, while the mTOR antagonist rapamycin promoted RCC cell apoptosis primarily through upregulation of HIF1α expression. Importantly, strong synergistic effects of MI-319 and rapamycin combinations at relatively low concentrations on RCC cell apoptosis were observed. Depletion of p53 or HIF1α impaired both antagonist-elicited apoptoses to differential extents, corresponding to their expression changes responding to chemical treatments, and double knockdown of p53 and HIF1α remarkably hindered MI-319- or rapamycin-induced apoptosis, suggesting that both p53 and HIF1α are involved in MDM2 or mTOR antagonist-induced apoptosis. Collectively, we propose that concurrent activation of p53 and HIF1α may effectively result in cancer-cell apoptosis, and that combined MDM2 antagonists and mTOR inhibitors may be useful in RCC therapy.Keywords: renal cell carcinoma, mTOR, MDM2, p53, HIF1α, apoptosishttps://www.dovepress.com/synergistic-roles-of-p53-and-hif1alpha-in-human-renal-cell-carcinoma-c-peer-reviewed-article-DDDTrenal cell carcinomamTORMDM2p53HIF1αapoptosis.
collection DOAJ
language English
format Article
sources DOAJ
author Liu QJ
Shen HL
Lin J
Xu XH
Ji ZG
Han X
Shang DH
Yang PQ
spellingShingle Liu QJ
Shen HL
Lin J
Xu XH
Ji ZG
Han X
Shang DH
Yang PQ
Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
Drug Design, Development and Therapy
renal cell carcinoma
mTOR
MDM2
p53
HIF1α
apoptosis.
author_facet Liu QJ
Shen HL
Lin J
Xu XH
Ji ZG
Han X
Shang DH
Yang PQ
author_sort Liu QJ
title Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
title_short Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
title_full Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
title_fullStr Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
title_full_unstemmed Synergistic roles of p53 and HIF1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mTOR and MDM2 signaling pathways
title_sort synergistic roles of p53 and hif1α in human renal cell carcinoma-cell apoptosis responding to the inhibition of mtor and mdm2 signaling pathways
publisher Dove Medical Press
series Drug Design, Development and Therapy
issn 1177-8881
publishDate 2016-02-01
description Qing-jun Liu,* Hong-liang Shen,* Jun Lin, Xiu-hong Xu, Zheng-guo Ji, Xiao Han, Dong-hao Shang, Pei-qian YangDepartment of Urology Surgery, Beijing Friendship Hospital, Capital Medical University, Beijing, People’s Republic of China*These authors contributed equally to this workIntroduction: mTOR and MDM2 signaling pathways are frequently deregulated in cancer development, and inhibition of mTOR or MDM2 independently enhances carcinoma-cell apoptosis. However, responses to mTOR and MDM2 antagonists in renal cell carcinoma (RCC) remain unknown.Materials and methods: A498 cells treated with MDM2 antagonist MI-319 and/or mTOR inhibitor rapamycin were employed in the present study. Cell apoptosis and Western blot analysis were performed.Results and conclusion: We found that the MDM2 inhibitor MI-319 induced RCC cell apoptosis mainly dependent on p53 overexpression, while the mTOR antagonist rapamycin promoted RCC cell apoptosis primarily through upregulation of HIF1α expression. Importantly, strong synergistic effects of MI-319 and rapamycin combinations at relatively low concentrations on RCC cell apoptosis were observed. Depletion of p53 or HIF1α impaired both antagonist-elicited apoptoses to differential extents, corresponding to their expression changes responding to chemical treatments, and double knockdown of p53 and HIF1α remarkably hindered MI-319- or rapamycin-induced apoptosis, suggesting that both p53 and HIF1α are involved in MDM2 or mTOR antagonist-induced apoptosis. Collectively, we propose that concurrent activation of p53 and HIF1α may effectively result in cancer-cell apoptosis, and that combined MDM2 antagonists and mTOR inhibitors may be useful in RCC therapy.Keywords: renal cell carcinoma, mTOR, MDM2, p53, HIF1α, apoptosis
topic renal cell carcinoma
mTOR
MDM2
p53
HIF1α
apoptosis.
url https://www.dovepress.com/synergistic-roles-of-p53-and-hif1alpha-in-human-renal-cell-carcinoma-c-peer-reviewed-article-DDDT
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