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Development of MK-8353, an orally administered ERK1/2 inhibitor, in patients with advanced solid tumors
- V体育2025版 - Moschos, Stergios J;
- Sullivan, Ryan J;
- Hwu, Wen-Jen;
- Ramanathan, Ramesh K (VSports注册入口);
- "V体育安卓版" Adjei, Alex A;
- V体育官网 - Fong, Peter C;
- Shapira-Frommer, Ronnie;
- VSports - Tawbi, Hussein A;
- Rubino, Joseph;
- Rush, Thomas S;
- "VSports" Zhang, Da;
- Miselis, Nathan R;
- VSports最新版本 - Samatar, Ahmed A;
- Chun, Patrick;
- Rubin, Eric H (VSports);
- Schiller, James;
- Long, Brian J (VSports手机版);
- Dayananth, Priya;
- "VSports手机版" Carr, Donna;
- Kirschmeier, Paul;
- Bishop, W Robert;
- Deng, Yongqi (VSports在线直播);
- "V体育安卓版" Cooper, Alan;
- Shipps, Gerald W;
- Moreno, Blanca Homet;
- Robert, Lidia (VSports最新版本);
- Ribas, Antoni;
- "VSports手机版" Flaherty, Keith T
- et al. (VSports最新版本)
Published Web Location
https://doi.org/10.1172/jci.insight.92352Abstract
Background
Constitutive activation of ERK1/2 occurs in various cancers, and its reactivation is a well-described resistance mechanism to MAPK inhibitors. ERK inhibitors may overcome the limitations of MAPK inhibitor blockade. The dual mechanism inhibitor SCH772984 has shown promising preclinical activity across various BRAFV600/RAS-mutant cancer cell lines and human cancer xenografts.Methods
We have developed an orally bioavailable ERK inhibitor, MK-8353; conducted preclinical studies to demonstrate activity, pharmacodynamic endpoints, dosing, and schedule; completed a study in healthy volunteers (P07652); and subsequently performed a phase I clinical trial in patients with advanced solid tumors (MK-8353-001). In the P07652 study, MK-8353 was administered as a single dose in 10- to 400-mg dose cohorts, whereas in the MK-8353-001 study, MK-8353 was administered in 100- to 800-mg dose cohorts orally twice daily. Safety, tolerability, pharmacokinetics, pharmacodynamics, and antitumor activity were analyzed."V体育官网入口" Results
MK-8353 exhibited comparable potency with SCH772984 across various preclinical cancer models. Forty-eight patients were enrolled in the P07652 study, and twenty-six patients were enrolled in the MK-8353-001 study. Adverse events included diarrhea (44%), fatigue (40%), nausea (32%), and rash (28%). Dose-limiting toxicity was observed in the 400-mg and 800-mg dose cohorts. Sufficient exposure to MK-8353 was noted that correlated with biological activity in preclinical data. Three of fifteen patients evaluable for treatment response in the MK-8353-001 study had partial response, all with BRAFV600-mutant melanomas.Conclusion
MK-8353 was well tolerated up to 400 mg twice daily and exhibited antitumor activity in patients with BRAFV600-mutant melanoma. However, antitumor activity was not particularly correlated with pharmacodynamic parameters.Trial registration (V体育平台登录)
ClinicalTrials.gov NCT01358331.Funding
Merck Sharp & Dohme Corp., a subsidiary of Merck & Co. Inc., and NIH (P01 CA168585 and R35 CA197633).Many UC-authored scholarly publications are freely available on this site because of the UC's open access policies VSports app下载. Let us know how this access is important for you.