A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib

PURPOSE: The MEK/MAPK pathway is commonly activated in HER2-positive breast cancer, but little investigation of targeting this pathway has been undertaken. Here we present the results of an in vitro preclinical evaluation of refametinib, an allosteric MEK1/2 inhibitor, in HER2-positive breast cancer...

Descripción completa

Detalles Bibliográficos
Autores principales: O’Shea, John, Cremona, Mattia, Morgan, Clare, Milewska, Malgorzata, Holmes, Frankie, Espina, Virginia, Liotta, Lance, O’Shaughnessy, Joyce, Toomey, Sinead, Madden, Stephen F., Carr, Aoife, Elster, Naomi, Hennessy, Bryan T., Eustace, Alex J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2017
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5689598/
https://www.ncbi.nlm.nih.gov/pubmed/29156708
http://dx.doi.org/10.18632/oncotarget.19461
_version_ 1783279413641609216
author O’Shea, John
Cremona, Mattia
Morgan, Clare
Milewska, Malgorzata
Holmes, Frankie
Espina, Virginia
Liotta, Lance
O’Shaughnessy, Joyce
Toomey, Sinead
Madden, Stephen F.
Carr, Aoife
Elster, Naomi
Hennessy, Bryan T.
Eustace, Alex J.
author_facet O’Shea, John
Cremona, Mattia
Morgan, Clare
Milewska, Malgorzata
Holmes, Frankie
Espina, Virginia
Liotta, Lance
O’Shaughnessy, Joyce
Toomey, Sinead
Madden, Stephen F.
Carr, Aoife
Elster, Naomi
Hennessy, Bryan T.
Eustace, Alex J.
author_sort O’Shea, John
collection PubMed
description PURPOSE: The MEK/MAPK pathway is commonly activated in HER2-positive breast cancer, but little investigation of targeting this pathway has been undertaken. Here we present the results of an in vitro preclinical evaluation of refametinib, an allosteric MEK1/2 inhibitor, in HER2-positive breast cancer cell lines including models of acquired resistance to trastuzumab or lapatinib. METHODS: A panel of HER2-positive breast cancer cells were profiled for mutational status and also for anti-proliferative response to refametinib alone and in combination with the PI3K inhibitor (PI3Ki) copanlisib and the HER2-targeted therapies trastuzumab and lapatinib. Reverse phase protein array (RPPA) was used to determine the effect of refametinib alone and in combination with PI3Ki and HER2-inhibitors on expression and phosphorylation of proteins in the PI3K/AKT and MEK/MAPK pathways. We validated our proteomic in vitro findings by utilising RPPA analysis of patients who received either trastuzumab, lapatinib or the combination of both drugs in the NCT00524303/LPT109096 clinical trial. RESULTS: Refametinib has anti-proliferative effects when used alone in 2/3 parental HER2-positive breast cancer cell lines (HCC1954, BT474), along with 3 models of these 2 cell lines with acquired trastuzumab or lapatinib resistance (6 cell lines tested). Refametinib treatment led to complete inhibition of MAPK signalling. In HCC1954, the most refametinib-sensitive cell line (IC(50) = 397 nM), lapatinib treatment inhibits phosphorylation of MEK and MAPK but activates AKT phosphorylation, in contrast to the other 2 parental cell lines tested (BT474-P, SKBR3-P), suggesting that HER2 may directly activate MEK/MAPK and not PI3K/AKT in HCC1954 cells but not in the other 2 cell lines, perhaps explaining the refametinib-sensitivity of this cell line. Using RPPA data from patients who received either trastuzumab, lapatinib or the combination of both drugs together with chemotherapy in the NCT00524303 clinical trial, we found that 18% (n=38) of tumours had decreased MAPK and increased AKT phosphorylation 14 days after treatment with HER2-targeted therapies. The combination of MEK inhibition (MEKi) with refametinib and copanlisib led to synergistic inhibition of growth in 4/6 cell lines tested (CI @ED(75) = 0.39-0.75), whilst the combinations of lapatinib and refametinib led to synergistic inhibition of growth in 3/6 cell lines (CI @ED(75) = 0.39-0.80). CONCLUSION: Refametinib alone or in combination with copanlisib or lapatinib could represent an improved treatment strategy for some patients with HER2-positive breast cancer, and should be considered for clinical trial evaluation. The direct down-regulation of MEK/MAPK but not AKT signalling by HER2 inhibition (e.g. by lapatinib or trastuzumab), which we demonstrate occurs in 18% of HER2-positive breast cancers may serve as a potential biomarker of responsiveness to the MEK inhibitor refametinib.
format Online
Article
Text
id pubmed-5689598
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Impact Journals LLC
record_format MEDLINE/PubMed
spelling pubmed-56895982017-11-17 A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib O’Shea, John Cremona, Mattia Morgan, Clare Milewska, Malgorzata Holmes, Frankie Espina, Virginia Liotta, Lance O’Shaughnessy, Joyce Toomey, Sinead Madden, Stephen F. Carr, Aoife Elster, Naomi Hennessy, Bryan T. Eustace, Alex J. Oncotarget Research Paper PURPOSE: The MEK/MAPK pathway is commonly activated in HER2-positive breast cancer, but little investigation of targeting this pathway has been undertaken. Here we present the results of an in vitro preclinical evaluation of refametinib, an allosteric MEK1/2 inhibitor, in HER2-positive breast cancer cell lines including models of acquired resistance to trastuzumab or lapatinib. METHODS: A panel of HER2-positive breast cancer cells were profiled for mutational status and also for anti-proliferative response to refametinib alone and in combination with the PI3K inhibitor (PI3Ki) copanlisib and the HER2-targeted therapies trastuzumab and lapatinib. Reverse phase protein array (RPPA) was used to determine the effect of refametinib alone and in combination with PI3Ki and HER2-inhibitors on expression and phosphorylation of proteins in the PI3K/AKT and MEK/MAPK pathways. We validated our proteomic in vitro findings by utilising RPPA analysis of patients who received either trastuzumab, lapatinib or the combination of both drugs in the NCT00524303/LPT109096 clinical trial. RESULTS: Refametinib has anti-proliferative effects when used alone in 2/3 parental HER2-positive breast cancer cell lines (HCC1954, BT474), along with 3 models of these 2 cell lines with acquired trastuzumab or lapatinib resistance (6 cell lines tested). Refametinib treatment led to complete inhibition of MAPK signalling. In HCC1954, the most refametinib-sensitive cell line (IC(50) = 397 nM), lapatinib treatment inhibits phosphorylation of MEK and MAPK but activates AKT phosphorylation, in contrast to the other 2 parental cell lines tested (BT474-P, SKBR3-P), suggesting that HER2 may directly activate MEK/MAPK and not PI3K/AKT in HCC1954 cells but not in the other 2 cell lines, perhaps explaining the refametinib-sensitivity of this cell line. Using RPPA data from patients who received either trastuzumab, lapatinib or the combination of both drugs together with chemotherapy in the NCT00524303 clinical trial, we found that 18% (n=38) of tumours had decreased MAPK and increased AKT phosphorylation 14 days after treatment with HER2-targeted therapies. The combination of MEK inhibition (MEKi) with refametinib and copanlisib led to synergistic inhibition of growth in 4/6 cell lines tested (CI @ED(75) = 0.39-0.75), whilst the combinations of lapatinib and refametinib led to synergistic inhibition of growth in 3/6 cell lines (CI @ED(75) = 0.39-0.80). CONCLUSION: Refametinib alone or in combination with copanlisib or lapatinib could represent an improved treatment strategy for some patients with HER2-positive breast cancer, and should be considered for clinical trial evaluation. The direct down-regulation of MEK/MAPK but not AKT signalling by HER2 inhibition (e.g. by lapatinib or trastuzumab), which we demonstrate occurs in 18% of HER2-positive breast cancers may serve as a potential biomarker of responsiveness to the MEK inhibitor refametinib. Impact Journals LLC 2017-07-22 /pmc/articles/PMC5689598/ /pubmed/29156708 http://dx.doi.org/10.18632/oncotarget.19461 Text en Copyright: © 2017 O’Shea et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0/) 3.0 (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
O’Shea, John
Cremona, Mattia
Morgan, Clare
Milewska, Malgorzata
Holmes, Frankie
Espina, Virginia
Liotta, Lance
O’Shaughnessy, Joyce
Toomey, Sinead
Madden, Stephen F.
Carr, Aoife
Elster, Naomi
Hennessy, Bryan T.
Eustace, Alex J.
A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title_full A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title_fullStr A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title_full_unstemmed A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title_short A preclinical evaluation of the MEK inhibitor refametinib in HER2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
title_sort preclinical evaluation of the mek inhibitor refametinib in her2-positive breast cancer cell lines including those with acquired resistance to trastuzumab or lapatinib
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5689598/
https://www.ncbi.nlm.nih.gov/pubmed/29156708
http://dx.doi.org/10.18632/oncotarget.19461
work_keys_str_mv AT osheajohn apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT cremonamattia apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT morganclare apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT milewskamalgorzata apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT holmesfrankie apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT espinavirginia apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT liottalance apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT oshaughnessyjoyce apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT toomeysinead apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT maddenstephenf apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT carraoife apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT elsternaomi apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT hennessybryant apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT eustacealexj apreclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT osheajohn preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT cremonamattia preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT morganclare preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT milewskamalgorzata preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT holmesfrankie preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT espinavirginia preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT liottalance preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT oshaughnessyjoyce preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT toomeysinead preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT maddenstephenf preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT carraoife preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT elsternaomi preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT hennessybryant preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib
AT eustacealexj preclinicalevaluationofthemekinhibitorrefametinibinher2positivebreastcancercelllinesincludingthosewithacquiredresistancetotrastuzumaborlapatinib

Ejemplares similares