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51 research outputs found

Efeito da sistematização sobre atributos físicos, químicos e biológicos de um solo de várzea no Rio Grande do Sul.

Author: A. Verstraete
F.K. Martens
H. Neels
J.C. Libeer
M. Deveaux
M. Van Damme
N. Devleeschouwer
P.E. Wallemacq
Publication venue: Pelotas: Embrapa Clima Temperado, 2014.
Publication date: 01/01/2004
Field of study

bitstream/item/110873/1/Boletim-189-web.pd

Sciensano Publications Repository

Ghent University Academic Bibliography

Institutional Repository Universiteit Antwerpen

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Photopatch testing

Repositório Institucional dos Hospitais da Universidade de Coimbra

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Steroid-free medium discloses oestrogenic effects of the bisphosphonate clodronate on breast cancer cells

Author: A Lipton
A Schmidt
AM Brodie
B Siwek
C Chaboteaux
C Harper-Wynne
C Harper-Wynne
E Demirpence
F Boccardo
F Journe
F Journe
F Journe
G Laurent
G Leclercq
H Fleisch
H Mouridsen
H Murakami
HL Neville-Webbe
HM Heshmati
IE Smith
IJ Diel
J Bonneterre
J Jensen
J-C Dumon
J-J Body
JC Frith
JH Lin
JJ Body
JM Nabholtz
K Villikka
L Myatt
LI Plotkin
M Baum
M Busch
M Sato
MV Lee
N Devleeschouwer
O Fromigue
PE Goss
PH Driggers
PJ Kushner
RE Coleman
RG Russell
RR Love
S Bardon
SG Senaratne
SP Jagdev
SP Luckman
SR Cummings
T Improta-Brears
T Osterman
T Powles
T Saarto
T Yoneda
TJ Powles
WR Miller
Z Zhao
Publication venue: Nature Publishing Group
Publication date: 01/11/2004
Field of study

SCOPUS: ar.jinfo:eu-repo/semantics/publishe

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PubMed Central

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Additive growth inhibitory effects of ibandronate and antiestrogens in estrogen receptor-positive breast cancer cell lines

INTRODUCTION: Bisphosphonates are inhibitors of osteoclast-mediated tumor-stimulated osteolysis, and they have become standard therapy for the management of bone metastases from breast cancer. These drugs can also directly induce growth inhibition and apoptosis of osteotropic cancer cells, including estrogen receptor-positive (ER+) breast cancer cells. METHODS: We examined the anti-proliferative properties of ibandronate on two ER+ breast cancer cell lines (MCF-7 and IBEP-2), and on one ER negative (ER-) cell line (MDA-MB-231). Experiments were performed in steroid-free medium to assess ER regulation and the effect of ibandronate in combination with estrogen or antiestrogens. RESULTS: Ibandronate inhibited cancer cell growth in a dose- and time-dependent manner (approximate IC(50): 10(-4 )M for MCF-7 and IBEP-2 cells; 3 × 10(-4 )M for MDA-MB-231 cells), partly through apoptosis induction. It completely abolished the mitogenic effect induced by 17β-estradiol in ER+ breast cancer cells, but affected neither ER regulation nor estrogen-induced progesterone receptor expression, as documented in MCF-7 cells. Moreover, ibandronate enhanced the growth inhibitory action of partial (4-hydroxytamoxifen) and pure (ICI 182,780, now called fluvestrant or Faslodex™) antiestrogens in estrogen-sensitive breast cancer cells. Combination analysis identified additive interactions between ibandronate and ER antagonists. CONCLUSION: These data constitute the first in vitro evidence for additive effects between ibandronate and antiestrogens, supporting their combined use for the treatment of bone metastases from breast cancer

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PubMed Central

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