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Epitranscriptomics & Cancer Adaptation : A.David

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Our research work focuses on the contribution of post-transcriptional mechanisms on cancer cell adaptation, in particular RNA epigenetic & translational control.

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Group name EquipeCTCS
Item Type Journal Article
Title Development of parallel reaction monitoring (PRM)-based quantitative proteomics applied to HER2-Positive breast cancer
Creator Guerin et al.
Author Mathilde Guerin
Author Yves Toiron
Author Emilie Baudelet
Author Matthieu Pophillat
Author Samuel Granjeaud
Author Patrick Fourquet
Author William Jacot
Author Carole Tarpin
Author Renaud Sabatier
Author Emilie Agavnian
Author Pascal Finetti
Author José Adelaide
Author Daniel Birnbaum
Author Christophe Ginestier
Author Emmanuelle Charafe-Jauffret
Author Patrice Viens
Author François Bertucci
Author Jean-Paul Borg
Author Luc Camoin
Abstract Introduction: treatments targeting the Human Epidermal Growth Factor Receptor 2 (HER2/ERBB2) have improved the natural history of HER2-positive breast cancer. However, except HER2 protein expression and gene amplification, there is no predictive biomarker to guide the HER2-targeted therapies. We developed Parallel reaction monitoring (PRM) a powerful approach, to quantify and evaluate key proteins involved in the HER2 pathway and/or anti-HER2 treatment sensitivity. Results: in BCLs, PRM measurements correlated with western blot immunocytochemistry and transcriptomic data. At baseline, higher expression of HER2, EGFR, PTEN and HER3 but lower expression of phospho-HER2 correlated with trastuzumab sensitivity. Under trastuzumab, PRM demonstrated a decrease in HER2 and an increase in phospho-HER2, which correlated with drug sensitivity. The opposite was observed under lapatinib. HER2 quantification was also correlated with immunohistochemistry in PDXs and clinical breast cancer samples. Discussion: in conclusion, PRM-based assay, developed to quantify proteins of the HER2 pathway in breast cancer samples revealed a large magnitude of expression, which may have relevance in terms of treatment sensitivity. Materials and Methods: we first evaluated PRM in term of sensitivity, linearity and reproducibility. PRM was then applied to breast cancer cell lines (BCLs) including BCLs exposed to anti-HER2 agents, patient-derived xenografts (PDXs) and frozen breast cancer samples.
Publication Oncotarget
Volume 9
Issue 73
Pages 33762-33777
Date Sep 18, 2018
Journal Abbr Oncotarget
Language eng
DOI 10.18632/oncotarget.26031
ISSN 1949-2553
Library Catalog PubMed
Extra PMID: 30333908 PMCID: PMC6173470
Tags breast cancer, HER2-positive, mass spectrometry, original, parallel reaction monitoring, proteomics
Date Added 2018/11/14 - 15:24:24
Date Modified 2019/05/14 - 18:23:59
Notes and Attachments PubMed entry (Attachment)


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