EGFR is required for FOS-dependent bone tumor development via RSK2/CREB signaling.
Markus LinderElisabeth GlitznerSriram SrivatsaLatifa BakiriKazuhiko MatsuokaParastoo ShahrouziMonika DumanicPhilipp NovoszelThomas MohrOliver LangerThomas WanekMarkus MitterhauserErwin F WagnerMaria SibiliaPublished in: EMBO molecular medicine (2019)
Osteosarcoma (OS) is a rare tumor of the bone occurring mainly in young adults accounting for 5% of all childhood cancers. Because of the limited therapeutic options, there has been no survival improvement for OS patients in the past 40 years. The epidermal growth factor receptor (EGFR) is highly expressed in OS; however, its clinical relevance is unclear. Here, we employed an autochthonous c-Fos-dependent OS mouse model (H2-c-fosLTR) and human OS tumor biopsies for preclinical studies aimed at identifying novel biomarkers and therapeutic benefits of anti-EGFR therapies. We show that EGFR deletion/inhibition results in reduced tumor formation in H2-c-fosLTR mice by directly inhibiting the proliferation of cancer-initiating osteoblastic cells by a mechanism involving RSK2/CREB-dependent c-Fos expression. Furthermore, OS patients with co-expression of EGFR and c-Fos exhibit reduced overall survival. Preclinical studies using human OS xenografts revealed that only tumors expressing both EGFR and c-Fos responded to anti-EGFR therapy demonstrating that c-Fos can be considered as a novel biomarker predicting response to anti-EGFR treatment in OS patients.
Keyphrases
- epidermal growth factor receptor
- tyrosine kinase
- small cell lung cancer
- advanced non small cell lung cancer
- end stage renal disease
- young adults
- ejection fraction
- mouse model
- chronic kidney disease
- endothelial cells
- poor prognosis
- newly diagnosed
- prognostic factors
- induced apoptosis
- bone mineral density
- type diabetes
- papillary thyroid
- stem cells
- patient reported outcomes
- long non coding rna
- bone loss
- cell death
- wild type
- vascular smooth muscle cells
- case control