TY - JOUR
T1 - A first-in-human phase I study to evaluate the MEK1/2 inhibitor, cobimetinib, administered daily in patients with advanced solid tumors
AU - Rosen, Lee S.
AU - LoRusso, Patricia
AU - Ma, Wen Wee
AU - Goldman, Jonathan W.
AU - Weise, Amy
AU - Colevas, A. Dimitrios
AU - Adjei, Alex
AU - Yazji, Salim
AU - Shen, Angela
AU - Johnston, Stuart
AU - Hsieh, Hsin Ju
AU - Chan, Iris T.
AU - Sikic, Branimir I.
N1 - Funding Information:
Lee S. Rosen, Patricia LoRusso, and Jonathan W. Goldman have received research funding from Genentech, Inc. Salim Yazji is a prior employee and current shareholder of Exelixis and is a current employee of Baxalta. Angela Shen is a prior employee of Exelixis and a current employee of Arvinas. Stuart Johnston is a shareholder and prior employee of Exelixis and a current employee of Nektar Therapeutics. Hsin-Ju Hsieh and Iris T. Chan are employees and shareholders of Roche. Branimir I. Sikic has received research funding from Exelixis, Genentech, Inc., Novartis, and Sanofi, and is a consultant for Novartis and Threshold Pharmaceuticals. Wen Wee Ma, Amy Weise, A. Dimitrios Colevas, and Alex Adjei declare that they have no potential conflicts of interest.
Funding Information:
The authors thank the patients and their families. This study was funded by Genentech, Inc. All authors participated in manuscript writing and approved the final version of the manuscript. We also acknowledge the contributions of Luna Musib, Steve Eppler, Alex de Crespigny, Jill Fredrickson, Mary Gates, and Yibing Yang. Editing and writing assistance was provided by Bryan Hains and Deborah Solymar (Genentech, Inc.) and was funded by Genentech, Inc.
Publisher Copyright:
© 2016, Springer Science+Business Media New York.
PY - 2016/10/1
Y1 - 2016/10/1
N2 - Objective Cobimetinib, a MEK1/2 inhibitor, was administered to patients with advanced solid tumors to assess safety, pharmacokinetics, pharmacodynamics, and anti-tumor activity. Methods For dose-escalation, a 3 + 3 design was used. Oral cobimetinib was administered once daily on a 21-day on/7-day off (21/7) or a 14-day on/14-day off (14/14) schedule. Serial plasma samples were collected for pharmacokinetic (PK) analysis on Day 1 and at steady state. In expansion stages, patients with RAS or RAF mutant tumors were treated at the maximum tolerated dose (MTD) of the 21/7 or 14/14 schedule. Results Ninety-seven patients received cobimetinib. In the 21/7 dose escalation, 36 patients enrolled in 8 cohorts (0.05 mg/kg–80 mg). Dose-limiting toxicities (DLTs) were Grade 4 hepatic encephalopathy, Grade 3 diarrhea, and Grade 3 rash. In the 14/14 dose escalation, 20 patients enrolled in 4 cohorts (60–125 mg). DLTs were Grade 3 rash and Grade 3 blurred vision associated with presence of reversible subretinal fluid. The MTD was 60 mg on 21/7 schedule and 100 mg on 14/14 schedule. Cobimetinib PK showed dose-proportional increases in exposure. The most frequent adverse events attributed to cobimetinib were diarrhea, rash, fatigue, edema, nausea, and vomiting. In patients treated at the 60-mg (21/7) or 100-mg (14/14) dose, one unconfirmed complete response and 6 confirmed partial responses were observed. All responses occurred in melanoma patients; 6 harbored the BRAFV600E mutation. Conclusions Cobimetinib is generally well tolerated and durable responses were observed in BRAFV600E mutant melanoma patients. Evaluation of cobimetinib in combination with other therapies is ongoing.
AB - Objective Cobimetinib, a MEK1/2 inhibitor, was administered to patients with advanced solid tumors to assess safety, pharmacokinetics, pharmacodynamics, and anti-tumor activity. Methods For dose-escalation, a 3 + 3 design was used. Oral cobimetinib was administered once daily on a 21-day on/7-day off (21/7) or a 14-day on/14-day off (14/14) schedule. Serial plasma samples were collected for pharmacokinetic (PK) analysis on Day 1 and at steady state. In expansion stages, patients with RAS or RAF mutant tumors were treated at the maximum tolerated dose (MTD) of the 21/7 or 14/14 schedule. Results Ninety-seven patients received cobimetinib. In the 21/7 dose escalation, 36 patients enrolled in 8 cohorts (0.05 mg/kg–80 mg). Dose-limiting toxicities (DLTs) were Grade 4 hepatic encephalopathy, Grade 3 diarrhea, and Grade 3 rash. In the 14/14 dose escalation, 20 patients enrolled in 4 cohorts (60–125 mg). DLTs were Grade 3 rash and Grade 3 blurred vision associated with presence of reversible subretinal fluid. The MTD was 60 mg on 21/7 schedule and 100 mg on 14/14 schedule. Cobimetinib PK showed dose-proportional increases in exposure. The most frequent adverse events attributed to cobimetinib were diarrhea, rash, fatigue, edema, nausea, and vomiting. In patients treated at the 60-mg (21/7) or 100-mg (14/14) dose, one unconfirmed complete response and 6 confirmed partial responses were observed. All responses occurred in melanoma patients; 6 harbored the BRAFV600E mutation. Conclusions Cobimetinib is generally well tolerated and durable responses were observed in BRAFV600E mutant melanoma patients. Evaluation of cobimetinib in combination with other therapies is ongoing.
KW - BRAF
KW - Cobimetinib
KW - MEK inhibitor
KW - Melanoma
KW - Phase I
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U2 - 10.1007/s10637-016-0374-3
DO - 10.1007/s10637-016-0374-3
M3 - Article
C2 - 27424159
AN - SCOPUS:84978884221
SN - 0167-6997
VL - 34
SP - 604
EP - 613
JO - Investigational New Drugs
JF - Investigational New Drugs
IS - 5
ER -