Publication | Open Access
Lessons learned from rindopepimut treatment in patients with EGFRvIII-expressing glioblastoma
32
Citations
10
References
2018
Year
PathologyHigh-grade GliomasCancer BiologyGliomaEgfr Exons 2–7Tumor BiologyNeuro-oncologyCancer Cell BiologyEgfrviii ArisesMolecular DiagnosticsRadiation OncologyNovel TherapyMolecular OncologyCancer ResearchTruncated Extracellular DomainMedicineCancer TreatmentCancer GeneticsPharmacologyCell BiologyRindopepimut TreatmentTumoral PathologyOncologyCell Development
EGFRvIII is the most common mutation of EGFR and results in the creation of a tumor-specific antigen that is detectable in 23–33% of human glioblastoma (GBM) (1). EGFRvIII arises due to the deletion of EGFR exons 2–7, which generates a truncated extracellular domain capable of constitutive EGFR activation.
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