Search CORE

6 research outputs found

Effects of dose modifications on the safety and efficacy of dacomitinib for EGFR mutation-positive non-small-cell lung cancer

Author: Corral-Jaime J. (Jesús)
Devgan G. (Geeta)
Lee K.H. (Ki Hyeong)
Linke R. (Rolf)
Migliorino M.R. (Maria Rita)
Mok T.S. (Tony S.)
Nakagawa K. (Kazuhiko)
Pluzanski A. (Adam)
Quinn S. (Susan)
Rosell R. (Rafael)
Tan W. (Weiwei)
Wang T. (Tao)
Wu Y.L. (Yi-Long)
Publication venue: 'Future Medicine Ltd'
Publication date: 01/01/2019
Field of study

Aim: We evaluated reasons for dacomitinib dose reduction (DR) and examined adverse event (AE) incidence, key efficacy end points (progression-free survival [PFS]/overall survival [OS]), and pharmacokinetics in dose-reducing patients in the ARCHER 1050 trial. Patients & methods: Newly diagnosed patients with EGFR mutation-positive, advanced non-small-cell lung cancer received oral dacomitinib (45 mg once-daily [QD]), with stepwise toxicity-managing DR (30 and 15 mg QD) permitted. Results: Skin toxicities (62.7%) were the most common DR-leading AEs. The AE incidence and severity decreased following DRs. Initial plasma dacomitinib exposure (45 mg QD) was generally lower in patients remaining at 45 mg QD compared with dose-reducing patients. Median PFS and OS were similar in all dacomitinib-treated patients and dose-reducing patients. Conclusion: Tolerability-guided dose modifications enabled patients to continue with dacomitinib and benefit from PFS/OS improvement

Universidad de Navarra

Dadun, University of Navarra

Global analysis of protein phosphorylation in yeast

Author: A Gruhler
AC Gavin
Angie S. Mah
Ashton Breitkreutz
Barry Schweitzer
BJ Breitkreutz
Brenda Andrews
CE Horak
Claudio De Virgilio
David F. Stern
EA Winzeler
G Manning
GD Bader
Geeta Devgan
Ghil Jona
Gregory Michaud
H Zhu
H Zhu
Heng Zhu
Hong Guo
HW Mewes
I Jonassen
I Xenarios
J Hanrahan
J Moffat
JA Ubersax
Jason Ptacek
Joseph Fasolo
Lihao Meng
M Huse
M Loog
Mark Gerstein
Martin C. Schmidt
Michael J. R. Stark
Michael Snyder
Mike Tyers
Najma Rachidi
P Cohen
P Uetz
Paul F. Predki
Rhonda R. McCartney
Richelle Sopko
S Ghaemmaghami
SB Ficarro
Soo-Jung Lee
T Ito
T Toda
TI Lee
WK Huh
X Pan
Xiaowei Zhu
Y Barral
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Stat3 as an Oncogene

Author: Chris Albanese
Geeta Devgan
Jacqueline F Bromberg
James E Darnell
Melissa H Wrzeszczynska
Richard G Pestell
Yanxiang Zhao
Publication venue: 'Elsevier BV'
Publication date
Field of study

Effects of dose modifications on the safety and efficacy of dacomitinib for EGFR mutation-positive non-small-cell lung cancer

Author: Corral-Jaime J. (Jesús)
Devgan G. (Geeta)
Lee K.H. (Ki Hyeong)
Linke R. (Rolf)
Migliorino M.R. (Maria Rita)
Mok T.S. (Tony S.)
Nakagawa K. (Kazuhiko)
Pluzanski A. (Adam)
Quinn S. (Susan)
Rosell R. (Rafael)
Tan W. (Weiwei)
Wang T. (Tao)
Wu Y.L. (Yi-Long)
Publication venue: 'Future Medicine Ltd'
Publication date: 01/01/2019
Field of study

Aim: We evaluated reasons for dacomitinib dose reduction (DR) and examined adverse event (AE) incidence, key efficacy end points (progression-free survival [PFS]/overall survival [OS]), and pharmacokinetics in dose-reducing patients in the ARCHER 1050 trial. Patients & methods: Newly diagnosed patients with EGFR mutation-positive, advanced non-small-cell lung cancer received oral dacomitinib (45 mg once-daily [QD]), with stepwise toxicity-managing DR (30 and 15 mg QD) permitted. Results: Skin toxicities (62.7%) were the most common DR-leading AEs. The AE incidence and severity decreased following DRs. Initial plasma dacomitinib exposure (45 mg QD) was generally lower in patients remaining at 45 mg QD compared with dose-reducing patients. Median PFS and OS were similar in all dacomitinib-treated patients and dose-reducing patients. Conclusion: Tolerability-guided dose modifications enabled patients to continue with dacomitinib and benefit from PFS/OS improvement

Universidad de Navarra

Stat3 as an Oncogene

Author: Adams
Alexander
Ausubel
Benitah
Besser
Boulton
Bromberg
Bromberg
Catlett-Falcone
Chen
Chris Albanese
Cory
Darnell
Garcia
Geeta Devgan
Grandis
Haspel
Hattori
Heinrich
Horvath
Jacqueline F Bromberg
James E Darnell
Kaplan
Kaplan
Kimura
Lee
Liu
Lodish
Matsumura
Melissa H Wrzeszczynska
Novak
Onishi
Richard G Pestell
Schaefer
Schulteis
Shuai
Stark
Takeda
Takeda
Takeda
Teglund
Tell
Thierfelder
Turkson
Udy
Vinkemeier
Wagner
Watowich
Weber-Nordt
Wen
Yanxiang Zhao
Yu
Zhong
Zhong
Zhu
Zong
Publication venue: 'Elsevier BV'
Publication date
Field of study

Global analysis of protein phosphorylation in yeast

Author: A Gruhler
AC Gavin
Angie S. Mah
Ashton Breitkreutz
Barry Schweitzer
BJ Breitkreutz
Brenda Andrews
CE Horak
Claudio De Virgilio
David F. Stern
EA Winzeler
G Manning
GD Bader
Geeta Devgan
Ghil Jona
Gregory Michaud
H Zhu
H Zhu
Heng Zhu
Hong Guo
HW Mewes
I Jonassen
I Xenarios
J Hanrahan
J Moffat
JA Ubersax
Jason Ptacek
Joseph Fasolo
Lihao Meng
M Huse
M Loog
Mark Gerstein
Martin C. Schmidt
Michael J. R. Stark
Michael Snyder
Mike Tyers
Najma Rachidi
P Cohen
P Uetz
Paul F. Predki
Rhonda R. McCartney
Richelle Sopko
S Ghaemmaghami
SB Ficarro
Soo-Jung Lee
T Ito
T Toda
TI Lee
WK Huh
X Pan
Xiaowei Zhu
Y Barral
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/12/2005
Field of study

University of Dundee Online Publications

core

core