Synapse - Genomic profiling of metastatic uveal melanoma and clinical results of a phase I study of the protein kinase C inhibitor AEB071

Genomic profiling of metastatic uveal melanoma and clinical results of a phase I study of the protein kinase C inhibitor AEB071 Journal Article

Authors:	Piperno-Neumann, S.; Larkin, J.; Carvajal, R. D.; Luke, J. J.; Schwartz, G. K.; Hodi, F. S.; Sablin, M. P.; Shoushtari, A. N.; Szpakowski, S.; Chowdhury, N. R.; Brannon, A. R.; Ramkumar, T.; de Koning, L.; Derti, A.; Emery, C.; Yerramilli-Rao, P.; Kapiteijn, E.
Article Title:	Genomic profiling of metastatic uveal melanoma and clinical results of a phase I study of the protein kinase C inhibitor AEB071
Abstract:	Up to 50% of patients with uveal melanoma (UM) develop metastatic disease, for which there is no effective systemic treatment. This study aimed to evaluate the safety and efficacy of the orally available protein kinase C inhibitor, AEB071, in patients with metastatic UM, and to perform genomic profiling of metastatic tumor samples, with the aim to propose combination therapies. Patients with metastatic UM (n = 153) were treated with AEB071 in a phase I, single-arm study. Patients received total daily doses of AEB071 ranging from 450 to 1,400 mg. First-cycle dose-limiting toxicities were observed in 13 patients (13%). These were most commonly gastrointestinal system toxicities and were dose related, occurring at doses ≥700 mg/day. Preliminary clinical activity was observed, with 3% of patients achieving a partial response and 50% with stable disease (median duration 15 weeks). High-depth, targeted next-generation DNA sequencing was performed on 89 metastatic tumor biopsy samples. Mutations previously identified in UM were observed, including mutations in GNAQ, GNA11, BAP1, SF3B1, PLCB4, and amplification of chromosome arm 8q. GNAQ/GNA11 mutations were observed at a similar frequency (93%) as previously reported, confirming a therapeutic window for inhibition of the downstream effector PKC in metastatic UM.In conclusion, the protein kinase C inhibitor AEB071 was well tolerated, and modest clinical activity was observed in metastatic UM. The genomic findings were consistent with previous reports in primary UM. Together, our data allow envisaging combination therapies of protein kinase C inhibitors with other compounds in metastatic UM. ©2020 American Association for Cancer Research.
Journal Title:	Molecular Cancer Therapeutics
Volume:	19
Issue:	4
ISSN:	1535-7163
Publisher:	American Association for Cancer Research
Date Published:	2020-04-01
Start Page:	1031
End Page:	1039
Language:	English
DOI:	10.1158/1535-7163.Mct-19-0098
PUBMED:	32029634
PROVIDER:	scopus
DOI/URL:	https://www.scopus.com/inward/record.uri?eid=2-s2.0-85082978978&doi=10.1158%2f1535-7163.MCT-19-0098&partnerID=40&md5=648d539401ac9b0f7c735bce3533480d
Notes:	Article -- Export Date: 1 May 2020 -- Source: Scopus

Altmetric

What is Altmetric?

Citation Impact

What is Dimensions Citation Badge?

BMJ Impact Analytics

MSK Authors

385 Schwartz
148 Carvajal
244 Shoushtari

Related MSK Work

Combined Pkc And Mek Inhibition In Uveal Melanoma With Gnaq And Gna11 Mutations

Oncogene 2014
The Phosphoinositide 3 Kinase A Selective Inhibitor Byl719 Enhances The Effect Of The Protein Kinase C Inhibitor Aeb071 In Gnaq/Gna11 Mutant Uveal Melanoma Cells

Molecular Cancer Therapeutics 2014
A Phase Ib Study Of Sotrastaurin, A Pkc Inhibitor, And Alpelisib, A Pi3 Kα Inhibitor, In Patients With Metastatic Uveal Melanoma

Cancers 2021
Treatment Of Uveal Melanoma

Cancer Treatment and Research 2016
Mutations In Gna11 In Uveal Melanoma

New England Journal of Medicine 2010