FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973

BACKGROUND: The BRAF inhibitor, vemurafenib, has recently been approved for the treatment of metastatic melanoma in patients harboring BRAF(V600) mutations. Currently, dual BRAF and MEK inhibition are ongoing in clinical trials with the goal of overcoming the acquired resistance that has unfortunate...

Descripción completa

Detalles Bibliográficos
Autores principales: Baudy, Andreas R, Dogan, Taner, Flores-Mercado, Judith E, Hoeflich, Klaus P, Su, Fei, van Bruggen, Nicholas, Williams, Simon-Peter
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer 2012
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3405466/
https://www.ncbi.nlm.nih.gov/pubmed/22651703
http://dx.doi.org/10.1186/2191-219X-2-22
_version_ 1782239142758842368
author Baudy, Andreas R
Dogan, Taner
Flores-Mercado, Judith E
Hoeflich, Klaus P
Su, Fei
van Bruggen, Nicholas
Williams, Simon-Peter
author_facet Baudy, Andreas R
Dogan, Taner
Flores-Mercado, Judith E
Hoeflich, Klaus P
Su, Fei
van Bruggen, Nicholas
Williams, Simon-Peter
author_sort Baudy, Andreas R
collection PubMed
description BACKGROUND: The BRAF inhibitor, vemurafenib, has recently been approved for the treatment of metastatic melanoma in patients harboring BRAF(V600) mutations. Currently, dual BRAF and MEK inhibition are ongoing in clinical trials with the goal of overcoming the acquired resistance that has unfortunately developed in some vemurafenib patients. FDG-PET measures of metabolic activity are increasingly employed as a pharmacodynamic biomarker for guiding single-agent or combination therapies by gauging initial drug response and monitoring disease progression. However, since tumors are inherently heterogeneous, investigating the effects of BRAF and MEK inhibition on FDG uptake in a panel of different melanomas could help interpret imaging outcomes. METHODS: (18) F-FDG uptake was measured in vitro in cells with wild-type and mutant (V600) BRAF, and in melanoma cells with an acquired resistance to vemurafenib. We treated the cells with vemurafenib alone or in combination with MEK inhibitor GDC-0973. PET imaging was used in mice to measure FDG uptake in A375 melanoma xenografts and in A375 R1, a vemurafenib-resistant derivative. Histological and biochemical studies of glucose transporters, the MAPK and glycolytic pathways were also undertaken. RESULTS: We demonstrate that vemurafenib is equally effective at reducing FDG uptake in cell lines harboring either heterozygous or homozygous BRAF(V600) but ineffective in cells with acquired resistance or having WT BRAF status. However, combination with GDC-0973 results in a highly significant increase of efficacy and inhibition of FDG uptake across all twenty lines. Drug-induced changes in FDG uptake were associated with altered levels of membrane GLUT-1, and cell lines harboring RAS mutations displayed enhanced FDG uptake upon exposure to vemurafenib. Interestingly, we found that vemurafenib treatment in mice bearing drug-resistant A375 xenografts also induced increased FDG tumor uptake, accompanied by increases in Hif-1α, Sp1 and Ksr protein levels. Vemurafenib and GDC-0973 combination efficacy was associated with decreased levels of hexokinase II, c-RAF, Ksr and p-MEK protein. CONCLUSIONS: We have demonstrated that (18) F-FDG-PET imaging reflects vemurafenib and GDC-0973 action across a wide range of metastatic melanomas. A delayed post-treatment increase in tumor FDG uptake should be considered carefully as it may well be an indication of acquired drug resistance. TRIAL REGISTRATION: ClinicalTrials.gov NCT01271803
format Online
Article
Text
id pubmed-3405466
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Springer
record_format MEDLINE/PubMed
spelling pubmed-34054662012-07-26 FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973 Baudy, Andreas R Dogan, Taner Flores-Mercado, Judith E Hoeflich, Klaus P Su, Fei van Bruggen, Nicholas Williams, Simon-Peter EJNMMI Res Original Research BACKGROUND: The BRAF inhibitor, vemurafenib, has recently been approved for the treatment of metastatic melanoma in patients harboring BRAF(V600) mutations. Currently, dual BRAF and MEK inhibition are ongoing in clinical trials with the goal of overcoming the acquired resistance that has unfortunately developed in some vemurafenib patients. FDG-PET measures of metabolic activity are increasingly employed as a pharmacodynamic biomarker for guiding single-agent or combination therapies by gauging initial drug response and monitoring disease progression. However, since tumors are inherently heterogeneous, investigating the effects of BRAF and MEK inhibition on FDG uptake in a panel of different melanomas could help interpret imaging outcomes. METHODS: (18) F-FDG uptake was measured in vitro in cells with wild-type and mutant (V600) BRAF, and in melanoma cells with an acquired resistance to vemurafenib. We treated the cells with vemurafenib alone or in combination with MEK inhibitor GDC-0973. PET imaging was used in mice to measure FDG uptake in A375 melanoma xenografts and in A375 R1, a vemurafenib-resistant derivative. Histological and biochemical studies of glucose transporters, the MAPK and glycolytic pathways were also undertaken. RESULTS: We demonstrate that vemurafenib is equally effective at reducing FDG uptake in cell lines harboring either heterozygous or homozygous BRAF(V600) but ineffective in cells with acquired resistance or having WT BRAF status. However, combination with GDC-0973 results in a highly significant increase of efficacy and inhibition of FDG uptake across all twenty lines. Drug-induced changes in FDG uptake were associated with altered levels of membrane GLUT-1, and cell lines harboring RAS mutations displayed enhanced FDG uptake upon exposure to vemurafenib. Interestingly, we found that vemurafenib treatment in mice bearing drug-resistant A375 xenografts also induced increased FDG tumor uptake, accompanied by increases in Hif-1α, Sp1 and Ksr protein levels. Vemurafenib and GDC-0973 combination efficacy was associated with decreased levels of hexokinase II, c-RAF, Ksr and p-MEK protein. CONCLUSIONS: We have demonstrated that (18) F-FDG-PET imaging reflects vemurafenib and GDC-0973 action across a wide range of metastatic melanomas. A delayed post-treatment increase in tumor FDG uptake should be considered carefully as it may well be an indication of acquired drug resistance. TRIAL REGISTRATION: ClinicalTrials.gov NCT01271803 Springer 2012-05-31 /pmc/articles/PMC3405466/ /pubmed/22651703 http://dx.doi.org/10.1186/2191-219X-2-22 Text en Copyright ©2012 Baudy et al.; licensee Springer. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research
Baudy, Andreas R
Dogan, Taner
Flores-Mercado, Judith E
Hoeflich, Klaus P
Su, Fei
van Bruggen, Nicholas
Williams, Simon-Peter
FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title_full FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title_fullStr FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title_full_unstemmed FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title_short FDG-PET is a good biomarker of both early response and acquired resistance in BRAF(V600) mutant melanomas treated with vemurafenib and the MEK inhibitor GDC-0973
title_sort fdg-pet is a good biomarker of both early response and acquired resistance in braf(v600) mutant melanomas treated with vemurafenib and the mek inhibitor gdc-0973
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3405466/
https://www.ncbi.nlm.nih.gov/pubmed/22651703
http://dx.doi.org/10.1186/2191-219X-2-22
work_keys_str_mv AT baudyandreasr fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT dogantaner fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT floresmercadojudithe fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT hoeflichklausp fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT sufei fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT vanbruggennicholas fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973
AT williamssimonpeter fdgpetisagoodbiomarkerofbothearlyresponseandacquiredresistanceinbrafv600mutantmelanomastreatedwithvemurafenibandthemekinhibitorgdc0973

Ejemplares similares