Epidermal growth factor signalling and bone metastasis

A Angelucci; A Citri; A De Luca; CT Guy; E Tian; G von Minckwitz; GD Roodman; GJ Powell; GR Mundy; J Zhu; JA Lorenzo; JB Johnston; K Wang; KJ Ibbotson; KL Weber; KR Hess; L Qin; LT Kelly; M Sibilia; M Wieduwilt; MR Schneider; N Normanno; N Normanno; N Takahashi; NE Hynes; P Khalili; PM Ravdin; R Brandt; RN Jorissen; S Yamazaki; S-i Harada; S-Y Chan; SJ Kim; TA Guise; WJ Boyle; WJ Muller; X Lu; X Lu; X Lu; Y Kang; Y Matsui

Epidermal growth factor signalling and bone metastasis

Authors: A Angelucci
A Citri
A De Luca
CT Guy
E Tian
G von Minckwitz
GD Roodman
GJ Powell
GR Mundy
J Zhu
JA Lorenzo
JB Johnston
K Wang
KJ Ibbotson
KL Weber
KR Hess
L Qin
LT Kelly
M Sibilia
M Wieduwilt
MR Schneider
N Normanno
N Normanno
N Takahashi
NE Hynes
P Khalili
PM Ravdin
R Brandt
RN Jorissen
S Yamazaki
S-i Harada
S-Y Chan
SJ Kim
TA Guise
WJ Boyle
WJ Muller
X Lu
X Lu
X Lu
Y Kang
Y Matsui
Publication date
Publisher: Nature Publishing Group
Doi

Abstract

Epidermal growth factor (EGF) signalling is well known for its multifaceted functions in development and tissue homoeostasis. The EGF family of ligands and receptors (ERBB family) have also been extensively investigated for their roles in promoting tumourigenesis and metastasis in a variety of cancer types. Recent findings indicate that EGF signalling is an important mediator of bone metastasis in breast, prostate and kidney cancers. The EGF signalling stimulates the growth of bone metastasis directly by increasing tumour cell proliferation and indirectly by engaging bone stromal cell in metastasis-promoting activities. Therefore, molecular targeting of ERBB receptors may benefit patients with bone metastasis and should be evaluated in clinical trials

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Last time updated on 11/12/2019