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Dive into the research topics where Roel P. Funke is active.

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Featured researches published by Roel P. Funke.


Journal of Thoracic Oncology | 2012

XL647—A Multitargeted Tyrosine Kinase Inhibitor: Results of a Phase II Study in Subjects with Non-small Cell Lung Cancer Who Have Progressed after Responding to Treatment with Either Gefitinib or Erlotinib

M. Catherine Pietanza; Thomas J. Lynch; Primo N. Lara; J. Cho; Ronald H. Yanagihara; Nandagopal Vrindavanam; Naveed Mahfooz Chowhan; Shirish M. Gadgeel; Nathan A. Pennell; Roel P. Funke; Ben Mitchell; Heather A. Wakelee; Vincent A. Miller

Introduction: Although patients with non-small cell lung cancer (NSCLC) whose tumors harbor epidermal growth factor receptor (EGFR) activating mutations commonly experience significant regressions when treated with erlotinib or gefitinib, they uniformly develop resistance to these agents. The secondary EGFR T790M mutation is found in 50% of patients with acquired resistance. Herein, we studied XL647, an oral small molecule inhibitor of multiple receptor tyrosine kinases, including EGFR, VEGFR2, HER2, and EphB4, in NSCLC patients known or suspected of having tumors harboring T790M. Methods: Eligible patients included those with relapsed or recurrent advanced NSCLC who progressed after ≥12 weeks of stable disease or response to erlotinib or gefitinib and/or those patients with a documented EGFR T790M. XL647 300 mg was administered once daily. The primary end point was objective response rate. Pretreatment plasma samples were collected for mutation testing of circulating tumor DNA. Results: Forty-one patients were enrolled; 33 were evaluable for efficacy. One partial response was observed (response rate 3% and 90% confidence interval, 0% to 14%). Of patients whose tumors harbored T790M, 67% (8/12) had progression of disease as best response compared with 14% (3/21) of those without this mutation. Plasma samples from 40 patients were available for mutation testing, 14 (35%) of which were found to have EGFR mutations. Conclusions: The 3% response rate observed did not meet the prespecified threshold to recommend further study of XL647 in patients who develop acquired resistance to erlotinib or gefitinib. Patients with T790M had a significantly worse progression-free survival.


Archive | 2003

MP53s AS MODIFIERS OF THE p53 PATHWAY AND METHODS OF USE

Marcia Belvin; Helen Francis-Lang; Lori Friedman; Gregory D. Plowman; Timothy S. Heuer; Danxi Li; Roel P. Funke


Archive | 2002

Modifiers of the p53 pathway and methods of use

Lori Friedman; Gregory D. Plowman; Marcia Belvin; Helen Francis-Lang; Danxi Li; Roel P. Funke


Archive | 2002

Slc7s as modifiers of the p53 pathway and methods of use

Lori Friedman; Gregory D. Plowman; Marcia Belvin; Helen Francis-Lang; Danxi Li; Roel P. Funke


Journal of Clinical Oncology | 2008

A phase I study of XL647, an EGFR, HER2, VEGFR2 inhibitor, administered orally daily to patients (pts) with advanced solid malignancies (ASM)

Heather A. Wakelee; J. M. Fehling; Julian R. Molina; Janet Lensing; Roel P. Funke; Dale Miles; B. I. Sikic


Archive | 2002

Lces as modifiers of the p53 pathway and methods of use

Lori Friedman; Gregory D. Plowman; Marcia Belvin; Helen Francis-Lang; Danxi Li; Roel P. Funke; Felix D. Karim; Linda N. Keyes; Thomas I. Koblizek


Archive | 2002

Modifier of the p53 pathway and methods of use

Marcia Belvin; Helen Francis-Lang; Gregory D. Plowman; Roel P. Funke; Danxi Li; Lori Friedman


Archive | 2007

HPRP4s Modifiers of the p53 Pathway and Methods of Use

Lori Friedman; Gregory D. Plowman; Tak Hung; Helen Francis-Lang; Danix Li; Roel P. Funke; Michael Costa


Archive | 2003

Rrp sequences and knockout mice and uses thereof

Helen Francis-Lang; Lori Friedman; Marcia Belvin; Gregory D. Plowman; Jeffrey S. Larson; Changyou Chen; Stephanie A. Roberston; Mario N. Lioubin; Wen Shi; Jocelyn Chan; Roel P. Funke; Danxi Li; Gunther Kauselmann; Hartmut Tintrup; Branko Zevnik; Michael Schoor; Brian John Reardon


Archive | 2002

IGS AS MODIFIERS OF THE P53 PATHWAY AND METHODS OF USE

Lori Friedman; Gregory D. Plowman; Marcia Belvin; Helen Francis-Lang; Danxi Li; Roel P. Funke; Mario N. Lioubin

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