Oncogene

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Oncogenic PTEN functions and models in T-cell malignancies
Oncogene - Tập 35 Số 30 - Trang 3887-3896 - 2016
Melania Tesio, Amélie Trinquand, Elizabeth Macintyre, Vahid Asnafi
NF-κB and STAT3 cooperatively induce IL6 in starved cancer cells
Oncogene - Tập 31 Số 29 - Trang 3467-3481 - 2012
Sarah Yoon, Sang‐Uk Woo, Jin-Ho Kang, Kiyoung Kim, Shin Hj, H-S Gwak, Sujin Park, Y-J Chwae
Evidence for mesenchymal-like sub-populations within squamous cell carcinomas possessing chemoresistance and phenotypic plasticity
Oncogene - Tập 29 - Trang 4170-4182 - 2010
D Basu, T-T K Nguyen, K T Montone, G Zhang, L-P Wang, J A Diehl, A K Rustgi, J T Lee, G S Weinstein, M Herlyn
Variable drug responses among malignant cells within individual tumors may represent a barrier to their eradication using chemotherapy. Carcinoma cells expressing mesenchymal markers resist conventional and epidermal growth factor receptor (EGFR)-targeted chemotherapy. In this study, we evaluated whether mesenchymal-like sub-populations within human squamous cell carcinomas (SCCs) with predominantly epithelial features contribute to overall therapy resistance. We identified a mesenchymal-like subset expressing low E-cadherin (Ecad-lo) and high vimentin within the upper aerodigestive tract SCCs. This subset was both isolated from the cell lines and was identified in xenografts and primary clinical specimens. The Ecad-lo subset contained more low-turnover cells, correlating with resistance to the conventional chemotherapeutic paclitaxel in vitro. Epidermal growth factor induced less stimulation of the mitogen-activated protein kinase and phosphatidylinositol-3-kinase pathways in Ecad-lo cells, which was likely due to lower EGFR expression in this subset and correlated with in vivo resistance to the EGFR-targeted antibody, cetuximab. The Ecad-lo and high E-cadherin subsets were dynamic in phenotype, showing the capacity to repopulate each other from single-cell clones. Taken together, these results provide evidence for a low-turnover, mesenchymal-like sub-population in SCCs with diminished EGFR pathway function and intrinsic resistance to conventional and EGFR-targeted chemotherapies.
Restoration of SHIP-1 activity in human leukemic cells modifies NF-κB activation pathway and cellular survival upon oxidative stress
Oncogene - Tập 25 Số 40 - Trang 5485-5494 - 2006
Geoffrey Gloire, Émilie Charlier, Souad Rahmouni, C. Volanti, Alain Chariot, Christophé Erneux, J Piette
Activated AKT regulates NF-κB activation, p53 inhibition and cell survival in HTLV-1-transformed cells
Oncogene - Tập 24 Số 44 - Trang 6719-6728 - 2005
Soo‐Jin Jeong, Cynthia A. Pise-Masison, Michael F. Radonovich, Hyeon Ung Park, John Brady
Drug discovery approaches targeting the PI3K/Akt pathway in cancer
Oncogene - Tập 27 Số 41 - Trang 5511-5526 - 2008
Carlos Garcı́a-Echeverrı́a, William R. Sellers
The Rb-family protein p107 inhibits translation by a PDK1-dependent mechanism
Oncogene - Tập 21 Số 51 - Trang 7891-7896 - 2002
Constantin Makris, Laure Voisin, Edith Giasson, Christopher Tudan, David R. Kaplan, Sylvain Meloche
Raft ceramide in molecular medicine
Oncogene - Tập 22 Số 45 - Trang 7070-7077 - 2003
Erich Gulbins, Richard Kolesnick
Inhibition of NADPH oxidase 4 activates apoptosis via the AKT/apoptosis signal-regulating kinase 1 pathway in pancreatic cancer PANC-1 cells
Oncogene - Tập 25 Số 26 - Trang 3699-3707 - 2006
Toshihiro Mochizuki, Shunsuke Furuta, Junji Mitsushita, Wenbin Shang, Masafumi Ito, Y. Yokoo, Maki Yamaura, Shinpachi Ishizone, Jun Nakayama, Ayano Konagai, Kunitaka Hirose, Kendo Kiyosawa, Tohru Kamata
NADPH oxidase 1 plays a critical mediating role in oncogenic Ras-induced vascular endothelial growth factor expression
Oncogene - Tập 27 Số 34 - Trang 4724-4732 - 2008
David E. Komatsu, Masayoshi Kato, Jun Nakayama, Shinichi Miyagawa, Tohru Kamata
Tổng số: 657   
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