Quantitative proteomics analysis identifies MUC1 as an effect sensor of EGFR inhibition.
H Rudolf de BoerMartin PoolEsméé JoostenMarieke EvertsDouwe F SamploniusWijnand HelfrichHarry J M GroenSuzanne van CootenFabrizia FusettiRudolf S N FehrmannElisabeth G E de VriesMarcel A T M van VugtPublished in: Oncogene (2018)
Tumor responses to cancer therapeutics are generally monitored every 2-3 months based on changes in tumor size. Dynamic biomarkers that reflect effective engagement of targeted therapeutics to the targeted pathway, so-called "effect sensors", would fulfill a need for non-invasive, drug-specific indicators of early treatment effect. Using a proteomics approach to identify effect sensors, we demonstrated MUC1 upregulation in response to epidermal growth factor receptor (EGFR)-targeting treatments in breast and lung cancer models. To achieve this, using semi-quantitative mass spectrometry, we found MUC1 to be significantly and durably upregulated in response to erlotinib, an EGFR-targeting treatment. MUC1 upregulation was regulated transcriptionally, involving PI3K-signaling and STAT3. We validated these results in erlotinib-sensitive human breast and non-small lung cancer cell lines. Importantly, erlotinib treatment of mice bearing SUM149 xenografts resulted in increased MUC1 shedding into plasma. Analysis of MUC1 using serial blood sampling may therefore be a new, relatively non-invasive tool to monitor early and drug-specific effects of EGFR-targeting therapeutics.
Keyphrases
- epidermal growth factor receptor
- tyrosine kinase
- advanced non small cell lung cancer
- mass spectrometry
- small cell lung cancer
- cancer therapy
- high resolution
- cell proliferation
- transcription factor
- squamous cell carcinoma
- endothelial cells
- poor prognosis
- type diabetes
- gene expression
- liquid chromatography
- genome wide
- metabolic syndrome
- combination therapy
- label free
- simultaneous determination
- capillary electrophoresis