Search CORE

1 research outputs found

E6-mediated activation of JNK drives EGFR signalling to promote proliferation and viral oncoprotein expression in cervical cancer

Author: A Bahrami
A Contreras-Paredes
A Macdonald
A Meixner
A Mialon
A Satsuka
AB Raitano
AHS Hall
B Zhang
BJ Pulverer
BL Bennett
C Cellurale
C He
C He
C Kuntzen
C Talora
C Tournier
Chemoradiotherapy for Cervical Cancer Meta-Analysis Collaboration.
CP Delury
CR Weston
CR Weston
CW Wasson
D Das
D Gaiotti
D Mili
D Pim
DO Moon
E Zhang
E-Y Kho
EJ Crosbie
EL Morgan
EL Morgan
EL Morgan
EL Morgan
F Rösl
F Varghese
F Wang
G Li
GA Rodrigues
GL Knight
H Hausen zur
I Pentland
I Vivanco
J de Wilde
J De-Castro Arce
J De-Castro Arce
J Li
JF Alcorn
JM Huibregtse
JM Spangle
JOM Bello
JY Zhang
K Butz
KJ Livak
L Xiao
L Zhao
LF Wetherill
LM Wang
M Humar
M Jiang
M Padash Barmchi
M Peto
M Scheffner
M Thomas
M-JM Chen
MA Bogoyevitch
N Chen
N Egawa
N Girnius
N Mine
NJ Kennedy
P Angel
Q-B She
R Eferl
R Ghittoni
R Qureshi
R Zenz
RA DeFilippis
S Detre
S Gupta
S Kyo
S Lee
S Mahata
S Miyauchi
S Morton
S Schumann
SK Sahu
SN Boyer
T Igaki
T Zhang
TM Brand
TP Cripe
V Purpura
X Liu
X Xie
Y Fang
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 10/12/2020
Field of study

Human papillomaviruses (HPV) are a major cause of malignancy worldwide, contributing to ~5% of all human cancers including almost all cases of cervical cancer and a growing number of ano-genital and oral cancers. HPV-induced malignancy is primarily driven by the viral oncogenes, E6 and E7, which manipulate host cellular pathways to increase cell proliferation and enhance cell survival, ultimately predisposing infected cells to malignant transformation. Consequently, a more detailed understanding of viral-host interactions in HPV-associated disease offers the potential to identify novel therapeutic targets. Here, we identify that the c-Jun N-terminal kinase (JNK) signalling pathway is activated in cervical disease and in cervical cancer. The HPV E6 oncogene induces JNK1/2 phosphorylation in a manner that requires the E6 PDZ binding motif. We show that blockade of JNK1/2 signalling using small molecule inhibitors, or knockdown of the canonical JNK substrate c-Jun, reduces cell proliferation and induces apoptosis in cervical cancer cells. We further demonstrate that this phenotype is at least partially driven by JNK-dependent activation of EGFR signalling via increased expression of EGFR and the EGFR ligands EGF and HB-EGF. JNK/c-Jun signalling promoted the invasive potential of cervical cancer cells and was required for the expression of the epithelial to mesenchymal transition (EMT)-associated transcription factor Slug and the mesenchymal marker Vimentin. Furthermore, JNK/c-Jun signalling is required for the constitutive expression of HPV E6 and E7, which are essential for cervical cancer cell growth and survival. Together, these data demonstrate a positive feedback loop between the EGFR signalling pathway and HPV E6/E7 expression, identifying a regulatory mechanism in which HPV drives EGFR signalling to promote proliferation, survival and EMT. Thus, our study has identified a novel therapeutic target that may be beneficial for the treatment of cervical cancer

Crossref

White Rose Research Online