Search CORE

56 research outputs found

CCI-779 (Temsirolimus) exhibits increased anti-tumor activity in low EGFR expressing HNSCC cell lines and is effective in cells with acquired resistance to cisplatin or cetuximab

Author: A Cassell
A Chawla
A Herzog
A Jimeno
A Stenzinger
AA Molinolo
AC Pickhard
Albrecht Stenzinger
DM Parkin
E Vilar
F Kamangar
F Nicolantonio Di
F Schedel
F Yang
FJ Kuppeveld van
Franziska Niehr
H Populo
Ingeborg Tinhofer
J Gilbert
JA Bonner
JD Coppock
JE Bauman
MA Gadhikar
MA Metwally
MG Fury
N Agrawal
N Aissat
N Stransky
O Ekshyyan
P Bossi
PC Ng
Q Li
R Krumbach
S Oiso
S Satheesha
SA Forbes
T Lu
TK Hoffmann
V D’Amato
V Endris
V Ramensky
VKU Grünwald
Volker Budach
VW Lui
Wilko Weichert
ZJ Sun
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Targeting the hedgehog transcription factors GLI1 and GLI2 restores sensitivity to vemurafenib-resistant human melanoma cells

Author: A Gonnissen
A L S A Vicente
A Lasfar
A Verfaillie
AD Steg
AD Steg
AM Chioni
AM Menzies
B Long
B Stecca
C R Goding
C Scapulatempo-Neto
C Sun
CA Brohem
CA Brohem
CM Johannessen
CM Johannessen
D Javelaud
D Javelaud
D Javelaud
D Javelaud
D K Alves-Fernandes
D Pan
DJ Konieczkowski
DR Green
DR Menon
F Debacq-Chainiaux
F Faiao-Flores
F Faião-Flores
F Niehr
F Sabbatino
Fedorenko IV
GV Long
GV Long
H Davies
H Tsao
H Yu
H Zhou
HX Fan
I Penna
I Ruiz
J Chauhan
J Lei
J Muller
J Sims-Mourtada
J Villanueva
J Villanueva
J Zavadil
J Zhou
JA Sosman
JK Chen
K Palle
K S Smalley
KC Queiroz
KH Paraiso
KH Paraiso
KS Hoek
KS Smalley
KS Smalley
KT Flaherty
KT Flaherty
L Huang
M Das Thakur
M Dugo
M Lauth
M Tauro
M Wickstrom
M Xu
MJ Pierrat
MP Matise
MP O'Connell
MR Girotti
MS Carlino
MS Ikram
N Wagle
NA Franken
P C Pennacchi
PC Pennacchi
PJ Eichhorn
R M Reis
R Nazarian
RE Meani
RK Gary
S Dennler
S Dennler
S Huang
S Narita
S S Maria-Engler
S Sandri
S Sandri
V L Vazquez
V Tirino
VI Alexaki
X Li
Y Fernandez
YH Fan
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

BRAF inhibitor (BRAFi) therapy for melanoma patients harboring the V600E mutation is initially highly effective, but almost all patients relapse within a few months. Understanding the molecular mechanisms underpinning BRAFi-based therapy is therefore an important issue. Here we identified a previously unsuspected mechanism of BRAFi resistance driven by elevated Hedgehog (Hh) pathway activation that is observed in a cohort of melanoma patients after vemurafenib treatment. Specifically, we demonstrate that melanoma cell lines, with acquired in vitro-induced vemurafenib resistance, show increased levels of glioma-associated oncogene homolog 1 and 2 (GLI1/GLI2) compared with naive cells. We also observed these findings in clinical melanoma specimens. Moreover, the increased expression of the transcription factors GLI1/GLI2 was independent of canonical Hh signaling and was instead correlated with the noncanonical Hh pathway, involving TGF beta/SMAD (transforming growth factor-beta/Sma- and Mad-related family) signaling. Knockdown of GLI1 and GLI2 restored sensitivity to vemurafenib-resistant cells, an effect associated with both growth arrest and senescence. Treatment of vemurafenib-resistant cells with the GLI1/GLI2 inhibitor Gant61 led to decreased invasion of the melanoma cells in a three-dimensional skin reconstruct model and was associated with a decrease in metalloproteinase (MMP2/MMP9) expression and microphthalmia transcription factor upregulation. Gant61 monotherapy did not alter the drug sensitivity of naive cells, but could reverse the resistance of melanoma cells chronically treated with vemurafenib. We further noted that alternating dosing schedules of Gant61 and vemurafenib prevented the onset of BRAFi resistance, suggesting that this could be a potential therapeutic strategy for the prevention of therapeutic escape. Our results suggest that targeting the Hh pathway in BRAFi-resistant melanoma may represent a viable therapeutic strategy to restore vemurafenib sensitivity, reducing or even inhibiting the acquired chemoresistance in melanoma patients.Fapesp-grant number 2012/04194-1, 2013/05172-4, 2014/24400-0 and 2015/10821-7, CNPq-grant number 150447/2013-2 and 471512/2013-3 and PRODOC-grant no 3193-32/2010. Work in the lab of KS Smalley was supported by the National Institutes of Health grants R01 CA161107, R21 CA198550, and Skin SPORE grant P50 CA168536info:eu-repo/semantics/publishedVersio

Universidade do Minho: RepositoriUM

Crossref

PubMed Central

Oxford University Research Archive

Bioenergetic modulation with dichloroacetate reduces the growth of melanoma cells and potentiates their response to BRAFV600E inhibition

Author: A Hall
Astrid L Basse
B Zheng
BM Madhok
C Dahl
Cecilie Abildgaard
Christina Dahl
D Baumunk
ED Michelakis
ED Michelakis
EM Dunbar
F Niehr
F Vazquez
H Davies
H Hur
H Shi
J Kaplon
J Kluza
J Robinson
J Tong
JN Sondergaard
JY Wong
K Kobayashi
LH Stockwin
M Buzzai
M Wu
MD Brand
MG Vander Heiden
MM de Barbi
O Warburg
P Corazao-Rozas
P Yuan
Per Guldberg
PW Stacpoole
PW Stacpoole
PW Stacpoole
R Esteve-Puig
R Haq
R Nazarian
RA Gatenby
RJ Gilbert
S Bonnet
Tao Ma
U Bergman
W Cao
YW Choi
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref