Lung cancer Erlotinib in unresectable non-small cell lung cancer when added to chemotherapy improves
overall survival by 19%, and improved
progression-free survival (PFS) by 29%, when compared to chemotherapy alone. The U.S.
Food and Drug Administration (FDA) approved erlotinib for the treatment of locally advanced or
metastatic non-small cell lung cancer that has failed at least one prior
chemotherapy regimen. In lung cancer, erlotinib has been shown to be effective in patients with or without EGFR mutations, but appears to be more effective in patients with EGFR mutations. Overall survival, progression-free survival and one-year survival are similar to standard second-line therapy (docetaxel or pemetrexed). Overall response rate is about 50% better than standard second-line chemotherapy.
Pancreatic cancer In November 2005, the FDA approved erlotinib in combination with
gemcitabine for treatment of locally advanced, unresectable, or metastatic
pancreatic cancer.
Resistance to treatment As with other ATP competitive small molecule tyrosine kinase inhibitors, such as
imatinib in
CML, patients rapidly develop resistance. In the case of erlotinib this typically occurs 8–12 months from the start of treatment. Over 50% of resistance is caused by a mutation in the ATP binding pocket of the EGFR kinase domain involving substitution of a small polar threonine residue with a large nonpolar methionine residue (
T790M). Approximately 20% of drug resistance is caused by amplification of the
hepatocyte growth factor receptor, which drives
ERBB3 dependent activation of
PI3K. ==Side effects==