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dc.contributor.authorSerra, V.
dc.contributor.authorScaltriti, M.
dc.contributor.authorPrudkin, L.
dc.contributor.authorEichhorn, Pieter
dc.contributor.authorIbrahim, Y.H.
dc.contributor.authorChandarlapaty, S.
dc.contributor.authorMarkman, B.
dc.contributor.authorRodriguez, O.
dc.contributor.authorGuzman, M.
dc.contributor.authorRodriguez, S.
dc.contributor.authorGili, M.
dc.contributor.authorRussillo, M.
dc.contributor.authorParra, J.L.
dc.contributor.authorSingh, S.
dc.contributor.authorArribas, J.
dc.contributor.authorRosen, N.
dc.contributor.authorBaselga, J.
dc.date.accessioned2020-12-03T02:54:09Z
dc.date.available2020-12-03T02:54:09Z
dc.date.issued2011
dc.identifier.citationSerra, V. and Scaltriti, M. and Prudkin, L. and Eichhorn, P.J.A. and Ibrahim, Y.H. and Chandarlapaty, S. and Markman, B. et al. 2011. PI3K inhibition results in enhanced HER signaling and acquired ERK dependency in HER2-overexpressing breast cancer. Oncogene. 30 (22): pp. 2547-2557.
dc.identifier.urihttp://hdl.handle.net/20.500.11937/81904
dc.identifier.doi10.1038/onc.2010.626
dc.description.abstract

There is a strong rationale to therapeutically target the phosphatidylinositol 3-kinase/protein kinase B/mammalian target of rapamycin (PI3K/AKT/mTOR) pathway in breast cancer since it is highly deregulated in this disease and it also mediates resistance to anti-HER2 therapies. However, initial studies with rapalogs, allosteric inhibitors of mTORC1, have resulted in limited clinical efficacy probably due to the release of a negative regulatory feedback loop that triggers AKT and ERK signaling. Since activation of AKT occurs via PI3K, we decided to explore whether PI3K inhibitors prevent the activation of these compensatory pathways. Using HER2-overexpressing breast cancer cells as a model, we observed that PI3K inhibitors abolished AKT activation. However, PI3K inhibition resulted in a compensatory activation of the ERK signaling pathway. This enhanced ERK signaling occurred as a result of activation of HER family receptors as evidenced by induction of HER receptors dimerization and phosphorylation, increased expression of HER3 and binding of adaptor molecules to HER2 and HER3. The activation of ERK was prevented with either MEK inhibitors or anti-HER2 monoclonal antibodies and tyrosine kinase inhibitors. Combined administration of PI3K inhibitors with either HER2 or MEK inhibitors resulted in decreased proliferation, enhanced cell death and superior anti-tumor activity compared with single agent PI3K inhibitors. Our findings indicate that PI3K inhibition in HER2-overexpressing breast cancer activates a new compensatory pathway that results in ERK dependency. Combined anti-MEK or anti-HER2 therapy with PI3K inhibitors may be required in order to achieve optimal efficacy in HER2-overexpressing breast cancer. This approach warrants clinical evaluation. © 2011 Macmillan Publishers Limited All rights reserved.

dc.languageEnglish
dc.publisherNATURE PUBLISHING GROUP
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/3.0/
dc.rights.uri
dc.subjectScience & Technology
dc.subjectLife Sciences & Biomedicine
dc.subjectBiochemistry & Molecular Biology
dc.subjectOncology
dc.subjectCell Biology
dc.subjectGenetics & Heredity
dc.subjectPI3K/mTOR
dc.subjectHER2
dc.subjectfeedback
dc.subjectERK
dc.subjectBEZ235
dc.subjectPHASE-II
dc.subjectTRASTUZUMAB RESISTANCE
dc.subjectPATHWAY ACTIVATION
dc.subjectANTITUMOR-ACTIVITY
dc.subjectPTEN
dc.subjectRECEPTOR
dc.subjectPIK3CA
dc.subjectMUTATIONS
dc.subjectGENE
dc.subjectMEK
dc.titlePI3K inhibition results in enhanced HER signaling and acquired ERK dependency in HER2-overexpressing breast cancer
dc.typeJournal Article
dcterms.source.volume30
dcterms.source.number22
dcterms.source.startPage2547
dcterms.source.endPage2557
dcterms.source.issn0950-9232
dcterms.source.titleOncogene
dc.date.updated2020-12-03T02:54:07Z
curtin.departmentSchool of Pharmacy and Biomedical Sciences
curtin.accessStatusOpen access
curtin.facultyFaculty of Health Sciences
curtin.contributor.orcidEichhorn, Pieter [0000-0001-5840-943X]
dcterms.source.eissn1476-5594
curtin.contributor.scopusauthoridEichhorn, Pieter [7004166602]


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