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Combined blockade of MEK and PI3KCA as an effective antitumor strategy in HER2 gene amplified human colorectal cancer models
by
Giunta, Emilio Francesco
, Ciardiello, Fortunato
, Morgillo, Floriana
, Matrone, Nunzia
, Troiani, Teresa
, Ciardiello, Davide
, Bracale, Umberto
, Napolitano, Stefania
, Belli, Valentina
, Migliardi, Giorgia
, Cottino, Francesca
, Bertotti, Andrea
, Martinelli, Erika
, De Falco, Vincenzo
, Trusolino, Livio
in
Antibodies
/ Apoptosis
/ Biomarkers
/ Biomedical and Life Sciences
/ Biomedicine
/ Cancer genetics
/ Cancer metastasis
/ Cancer Research
/ Cancer therapies
/ Cancer treatment
/ Care and treatment
/ Chemotherapy
/ Clinical medicine
/ Clinical trials
/ Colorectal cancer
/ Epidermal growth factor
/ Epidermal growth factors
/ Gene amplification
/ Genes
/ Genetic aspects
/ HER2-amplified cancer
/ Immunoglobulins
/ Immunology
/ Kinase inhibitors
/ Kinases
/ Lung cancer
/ MEK and PI3KCA inhibitors; xenografts; patient-derived xenografts
/ Monoclonal antibodies
/ Mutation
/ Oncology
/ Patients
/ Phosphatidylinositol phosphates
/ Retirement benefits
/ Targeted cancer therapy
/ Tumors
2019
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Combined blockade of MEK and PI3KCA as an effective antitumor strategy in HER2 gene amplified human colorectal cancer models
by
Giunta, Emilio Francesco
, Ciardiello, Fortunato
, Morgillo, Floriana
, Matrone, Nunzia
, Troiani, Teresa
, Ciardiello, Davide
, Bracale, Umberto
, Napolitano, Stefania
, Belli, Valentina
, Migliardi, Giorgia
, Cottino, Francesca
, Bertotti, Andrea
, Martinelli, Erika
, De Falco, Vincenzo
, Trusolino, Livio
in
Antibodies
/ Apoptosis
/ Biomarkers
/ Biomedical and Life Sciences
/ Biomedicine
/ Cancer genetics
/ Cancer metastasis
/ Cancer Research
/ Cancer therapies
/ Cancer treatment
/ Care and treatment
/ Chemotherapy
/ Clinical medicine
/ Clinical trials
/ Colorectal cancer
/ Epidermal growth factor
/ Epidermal growth factors
/ Gene amplification
/ Genes
/ Genetic aspects
/ HER2-amplified cancer
/ Immunoglobulins
/ Immunology
/ Kinase inhibitors
/ Kinases
/ Lung cancer
/ MEK and PI3KCA inhibitors; xenografts; patient-derived xenografts
/ Monoclonal antibodies
/ Mutation
/ Oncology
/ Patients
/ Phosphatidylinositol phosphates
/ Retirement benefits
/ Targeted cancer therapy
/ Tumors
2019
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Combined blockade of MEK and PI3KCA as an effective antitumor strategy in HER2 gene amplified human colorectal cancer models
by
Giunta, Emilio Francesco
, Ciardiello, Fortunato
, Morgillo, Floriana
, Matrone, Nunzia
, Troiani, Teresa
, Ciardiello, Davide
, Bracale, Umberto
, Napolitano, Stefania
, Belli, Valentina
, Migliardi, Giorgia
, Cottino, Francesca
, Bertotti, Andrea
, Martinelli, Erika
, De Falco, Vincenzo
, Trusolino, Livio
in
Antibodies
/ Apoptosis
/ Biomarkers
/ Biomedical and Life Sciences
/ Biomedicine
/ Cancer genetics
/ Cancer metastasis
/ Cancer Research
/ Cancer therapies
/ Cancer treatment
/ Care and treatment
/ Chemotherapy
/ Clinical medicine
/ Clinical trials
/ Colorectal cancer
/ Epidermal growth factor
/ Epidermal growth factors
/ Gene amplification
/ Genes
/ Genetic aspects
/ HER2-amplified cancer
/ Immunoglobulins
/ Immunology
/ Kinase inhibitors
/ Kinases
/ Lung cancer
/ MEK and PI3KCA inhibitors; xenografts; patient-derived xenografts
/ Monoclonal antibodies
/ Mutation
/ Oncology
/ Patients
/ Phosphatidylinositol phosphates
/ Retirement benefits
/ Targeted cancer therapy
/ Tumors
2019
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Combined blockade of MEK and PI3KCA as an effective antitumor strategy in HER2 gene amplified human colorectal cancer models
Journal Article
Combined blockade of MEK and PI3KCA as an effective antitumor strategy in HER2 gene amplified human colorectal cancer models
2019
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Overview
Background
Targeting the epidermal growth factor receptor (EGFR) either alone or in combination with chemotherapy is an effective treatment for patients with
RAS
wild-type metastatic colorectal cancer (mCRC). However, only a small percentage of mCRC patients receive clinical benefits from anti-EGFR therapies, due to the development of resistance mechanisms. In this regard, HER2 has emerged as an actionable target in the treatment of mCRC patients with resistance to anti-EGFR therapy.
Methods
We have used SW48 and LIM1215 human colon cancer cell lines, quadruple wild-type for
KRAS, NRAS, BRAF
and
PI3KCA
genes, and their
HER2
–amplified (LIM1215-HER2 and SW48-HER2) derived cells to perform in vitro and in vivo studies in order to identify novel therapeutic strategies in
HER2
gene amplified human colorectal cancer.
Results
LIM1215-HER2 and SW48-HER2 cells showed over-expression and activation of the HER family receptors and concomitant intracellular downstream signaling including the pro-survival PI3KCA/AKT and the mitogenic RAS/RAF/MEK/MAPK pathways.
HER2
-amplified cells were treated with several agents including anti-EGFR antibodies (cetuximab, SYM004 and MM151); anti-HER2 (trastuzumab, pertuzumab and lapatinib) inhibitors; anti-HER3 (duligotuzumab) inhibitors; and MEK and PI3KCA inhibitors, such as refametinib and pictilisib, as single agents and in combination. Subsequently, different in vivo experiments have been performed. MEK plus PI3KCA inhibitors treatment determined the best antitumor activity. These results were validated in vivo in
HER2
-amplified patient derived tumor xenografts from three metastatic colorectal cancer patients.
Conclusions
These results suggest that combined therapy with MEK and PI3KCA inhibitors could represent a novel and effective treatment option for
HER2
-amplified colorectal cancer.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
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