In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma

Ileine M. Sanchez; Timothy J. Purwin; Inna Chervoneva; Dan A. Erkes; Mai Q. Nguyen; Michael A. Davies; Katherine L. Nathanson; Kristel Kemper; Daniel S. Peeper; Andrew E. Aplin

doi:10.1158/1535-7163.MCT-18-1056

In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma

Ileine M. Sanchez, Timothy J. Purwin, Inna Chervoneva, Dan A. Erkes, Mai Q. Nguyen, Michael A. Davies, Katherine L. Nathanson, Kristel Kemper, Daniel S. Peeper, Andrew E. Aplin

Melanoma Medical Oncology

Research output: Contribution to journal › Article › peer-review

13 Scopus citations

Abstract

Combined BRAF and MEK inhibition is a standard of care in patients with advanced BRAF-mutant melanoma, but acquired resistance remains a challenge that limits response durability. Here, we quantitated in vivo ERK1/2 activity and tumor response associated with resistance to combined BRAF and MEK inhibition in mutant BRAF xenografts. We found that ERK1/2 pathway reactivation preceded the growth of resistant tumors. Moreover, we detected a subset of cells that not only persisted throughout long-term treatment but restored ERK1/ 2 signaling and grew upon drug removal. Cell lines derived from combination-resistant tumors (CRT) exhibited elevated ERK1/2 phosphorylation, which were sensitive to ERK1/2 inhibition. In some CRTs, we detected a tandem duplication of the BRAF kinase domain. Monitoring ERK1/2 activity in vivo was efficacious in predicting tumor response during intermittent treatment. We observed maintained expression of the mitotic regulator, polo-like kinase 1 (Plk1), in melanoma resistant to BRAF and MEK inhibitors. Plk1 inhibition induced apoptosis in CRTs, leading to slowed growth of BRAF and MEK inhibitor–resistant tumors in vivo. These data demonstrate the utility of in vivo ERK1/2 pathway reporting as a tool to optimize clinical dosing schemes and establish suppression of Plk1 as potential salvage therapy for BRAF inhibitor and MEK inhibitor–resistant melanoma.

Original language	English (US)
Pages (from-to)	1637-1648
Number of pages	12
Journal	Molecular cancer therapeutics
Volume	18
Issue number	9
DOIs	https://doi.org/10.1158/1535-7163.MCT-18-1056
State	Published - 2019

ASJC Scopus subject areas

Oncology
Cancer Research

MD Anderson CCSG core facilities

Bioinformatics Shared Resource
Functional Proteomics Reverse Phase Protein Array Core

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10.1158/1535-7163.MCT-18-1056

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Sanchez, I. M., Purwin, T. J., Chervoneva, I., Erkes, D. A., Nguyen, M. Q., Davies, M. A., Nathanson, K. L., Kemper, K., Peeper, D. S., & Aplin, A. E. (2019). In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma. Molecular cancer therapeutics, 18(9), 1637-1648. https://doi.org/10.1158/1535-7163.MCT-18-1056

@article{3be1b196c7844b46a8f2ff30c34e631d,

title = "In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma",

abstract = "Combined BRAF and MEK inhibition is a standard of care in patients with advanced BRAF-mutant melanoma, but acquired resistance remains a challenge that limits response durability. Here, we quantitated in vivo ERK1/2 activity and tumor response associated with resistance to combined BRAF and MEK inhibition in mutant BRAF xenografts. We found that ERK1/2 pathway reactivation preceded the growth of resistant tumors. Moreover, we detected a subset of cells that not only persisted throughout long-term treatment but restored ERK1/ 2 signaling and grew upon drug removal. Cell lines derived from combination-resistant tumors (CRT) exhibited elevated ERK1/2 phosphorylation, which were sensitive to ERK1/2 inhibition. In some CRTs, we detected a tandem duplication of the BRAF kinase domain. Monitoring ERK1/2 activity in vivo was efficacious in predicting tumor response during intermittent treatment. We observed maintained expression of the mitotic regulator, polo-like kinase 1 (Plk1), in melanoma resistant to BRAF and MEK inhibitors. Plk1 inhibition induced apoptosis in CRTs, leading to slowed growth of BRAF and MEK inhibitor–resistant tumors in vivo. These data demonstrate the utility of in vivo ERK1/2 pathway reporting as a tool to optimize clinical dosing schemes and establish suppression of Plk1 as potential salvage therapy for BRAF inhibitor and MEK inhibitor–resistant melanoma.",

author = "Sanchez, {Ileine M.} and Purwin, {Timothy J.} and Inna Chervoneva and Erkes, {Dan A.} and Nguyen, {Mai Q.} and Davies, {Michael A.} and Nathanson, {Katherine L.} and Kristel Kemper and Peeper, {Daniel S.} and Aplin, {Andrew E.}",

note = "Funding Information: A.E. Aplin is supported by NIH R01 awards CA160495 and CA182365 and by Dr. Miriam and Sheldon G. Adelson Medical Research Foundation. I. Sanchez is supported by a diversity supplement to CA160495. The Sidney Kimmel Cancer Center Flow Cytometry, Translational Pathology, and Meta-Omics core facilities are supported by an NIH/NCI Support Grant (P30 CA056036). The RPPA studies were performed at the Functional Proteomics Core Facility at The University of Texas MD Anderson Cancer Center (Houston, TX), which is supported by an NCI Cancer Center Support Grant (CA16672). Funding Information: M.A. Davies reports receiving a commercial research grant from AstraZe-neca, Roche-Genentech, GSK, and Sanofi-Aventis and is a consultant/advisory board member for GSK, Roche-Genentech, Novartis, Array, and Sanofi-Aventis. A.E. Aplin reports receiving a commercial research grant from Pfizer and is a consultant/advisory board member for SpringWorks Therapeutics and Fortress Biotech. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2019 American Association for Cancer Research.",

year = "2019",

doi = "10.1158/1535-7163.MCT-18-1056",

language = "English (US)",

volume = "18",

pages = "1637--1648",

journal = "Molecular cancer therapeutics",

issn = "1535-7163",

publisher = "American Association for Cancer Research Inc.",

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T1 - In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma

AU - Sanchez, Ileine M.

AU - Purwin, Timothy J.

AU - Chervoneva, Inna

AU - Erkes, Dan A.

AU - Nguyen, Mai Q.

AU - Davies, Michael A.

AU - Nathanson, Katherine L.

AU - Kemper, Kristel

AU - Peeper, Daniel S.

AU - Aplin, Andrew E.

N1 - Funding Information: A.E. Aplin is supported by NIH R01 awards CA160495 and CA182365 and by Dr. Miriam and Sheldon G. Adelson Medical Research Foundation. I. Sanchez is supported by a diversity supplement to CA160495. The Sidney Kimmel Cancer Center Flow Cytometry, Translational Pathology, and Meta-Omics core facilities are supported by an NIH/NCI Support Grant (P30 CA056036). The RPPA studies were performed at the Functional Proteomics Core Facility at The University of Texas MD Anderson Cancer Center (Houston, TX), which is supported by an NCI Cancer Center Support Grant (CA16672). Funding Information: M.A. Davies reports receiving a commercial research grant from AstraZe-neca, Roche-Genentech, GSK, and Sanofi-Aventis and is a consultant/advisory board member for GSK, Roche-Genentech, Novartis, Array, and Sanofi-Aventis. A.E. Aplin reports receiving a commercial research grant from Pfizer and is a consultant/advisory board member for SpringWorks Therapeutics and Fortress Biotech. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: © 2019 American Association for Cancer Research.

PY - 2019

Y1 - 2019

N2 - Combined BRAF and MEK inhibition is a standard of care in patients with advanced BRAF-mutant melanoma, but acquired resistance remains a challenge that limits response durability. Here, we quantitated in vivo ERK1/2 activity and tumor response associated with resistance to combined BRAF and MEK inhibition in mutant BRAF xenografts. We found that ERK1/2 pathway reactivation preceded the growth of resistant tumors. Moreover, we detected a subset of cells that not only persisted throughout long-term treatment but restored ERK1/ 2 signaling and grew upon drug removal. Cell lines derived from combination-resistant tumors (CRT) exhibited elevated ERK1/2 phosphorylation, which were sensitive to ERK1/2 inhibition. In some CRTs, we detected a tandem duplication of the BRAF kinase domain. Monitoring ERK1/2 activity in vivo was efficacious in predicting tumor response during intermittent treatment. We observed maintained expression of the mitotic regulator, polo-like kinase 1 (Plk1), in melanoma resistant to BRAF and MEK inhibitors. Plk1 inhibition induced apoptosis in CRTs, leading to slowed growth of BRAF and MEK inhibitor–resistant tumors in vivo. These data demonstrate the utility of in vivo ERK1/2 pathway reporting as a tool to optimize clinical dosing schemes and establish suppression of Plk1 as potential salvage therapy for BRAF inhibitor and MEK inhibitor–resistant melanoma.

AB - Combined BRAF and MEK inhibition is a standard of care in patients with advanced BRAF-mutant melanoma, but acquired resistance remains a challenge that limits response durability. Here, we quantitated in vivo ERK1/2 activity and tumor response associated with resistance to combined BRAF and MEK inhibition in mutant BRAF xenografts. We found that ERK1/2 pathway reactivation preceded the growth of resistant tumors. Moreover, we detected a subset of cells that not only persisted throughout long-term treatment but restored ERK1/ 2 signaling and grew upon drug removal. Cell lines derived from combination-resistant tumors (CRT) exhibited elevated ERK1/2 phosphorylation, which were sensitive to ERK1/2 inhibition. In some CRTs, we detected a tandem duplication of the BRAF kinase domain. Monitoring ERK1/2 activity in vivo was efficacious in predicting tumor response during intermittent treatment. We observed maintained expression of the mitotic regulator, polo-like kinase 1 (Plk1), in melanoma resistant to BRAF and MEK inhibitors. Plk1 inhibition induced apoptosis in CRTs, leading to slowed growth of BRAF and MEK inhibitor–resistant tumors in vivo. These data demonstrate the utility of in vivo ERK1/2 pathway reporting as a tool to optimize clinical dosing schemes and establish suppression of Plk1 as potential salvage therapy for BRAF inhibitor and MEK inhibitor–resistant melanoma.

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In vivo ERK1/2 reporter predictively models response and resistance to combined BRAF and MEK inhibitors in melanoma

Abstract

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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