PloS one, 2015-03, Vol.10 (3), p.e0119135-e0119135
2015
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- Autor(en) / Beteiligte
- Titel
- Chloroquine enhances gefitinib cytotoxicity in gefitinib-resistant nonsmall cell lung cancer cells
- Ist Teil von
- PloS one, 2015-03, Vol.10 (3), p.e0119135-e0119135
- Ort / Verlag
- United States: Public Library of Science
- Erscheinungsjahr
- 2015
- Quelle
- MEDLINE
- Beschreibungen/Notizen
- Epidermal growth factor receptor tyrosine kinase inhibitors (EGFR-TKIs), including gefitinib, are effective for non-small cell lung cancer (NSCLC) patients with EGFR mutations. However, these patients eventually develop resistance to EGFR-TKI. The goal of the present study was to investigate the involvement of autophagy in gefitinib resistance. We developed gefitinib-resistant cells (PC-9/gef) from PC-9 cells (containing exon 19 deletion EGFR) after long-term exposure in gefitinib. PC-9/gef cells (B4 and E3) were 200-fold more resistant to gefitinib than PC-9/wt cells. Compared with PC-9/wt cells, both PC-9/gefB4 and PC-9/gefE3 cells demonstrated higher basal LC3-II levels which were inhibited by 3-methyladenine (3-MA, an autophagy inhibitor) and potentiated by chloroquine (CQ, an inhibitor of autophagolysosomes formation), indicating elevated autophagy in PC-9/gef cells. 3-MA and CQ concentration-dependently inhibited cell survival of both PC-9wt and PC-9/gef cells, suggesting that autophagy may be pro-survival. Furthermore, gefitinib increased LC3-II levels and autolysosome formation in both PC-9/wt cells and PC-9/gef cells. In PC-9/wt cells, CQ potentiated the cytotoxicity by low gefitinib (3 nM). Moreover, CQ overcame the acquired gefitinib resistance in PC-9/gef cells by enhancing gefitinib-induced cytotoxicity, activation of caspase 3 and poly (ADP-ribose) polymerase cleavage. Using an in vivo model xenografting with PC-9/wt and PC-9/gefB4 cells, oral administration of gefitinib (50 mg/kg) completely inhibited the tumor growth of PC-9/wt but not PC-9/gefB4cells. Combination of CQ (75 mg/kg, i.p.) and gefitinib was more effective than gefitinib alone in reducing the tumor growth of PC-9/gefB4. Our data suggest that inhibition of autophagy may be a therapeutic strategy to overcome acquired resistance of gefitinib in EGFR mutation NSCLC patients.
- Sprache
- Englisch
- Identifikatoren
- ISSN: 1932-6203eISSN: 1932-6203DOI: 10.1371/journal.pone.0119135Titel-ID: cdi_plos_journals_1666740913
- Format
- –
- Schlagworte
- Adenine - analogs & derivatives, Adenine - pharmacology, Adenosine diphosphate, Antineoplastic Agents - pharmacology, Antineoplastic Agents - therapeutic use, Apoptosis, Autophagy, Autophagy - drug effects, Biocompatibility, Cancer, Cancer therapies, Carcinoma, Non-Small-Cell Lung - drug therapy, Carcinoma, Non-Small-Cell Lung - genetics, Carcinoma, Non-Small-Cell Lung - pathology, Caspase, Caspase-3, Cell death, Cell Line, Tumor, Cell survival, Chloroquine, Chloroquine - pharmacology, Chloroquine - therapeutic use, Clonal deletion, Cytotoxicity, Epidermal growth factor, Epidermal growth factor receptors, Gefitinib, Humans, Inhibitor drugs, Inhibitors, Kinases, Lung cancer, Lung diseases, Lung Neoplasms - drug therapy, Lung Neoplasms - genetics, Lung Neoplasms - pathology, Mutation, Non-small cell lung cancer, Non-small cell lung carcinoma, Oral administration, Patients, Phagocytosis, Protein-tyrosine kinase receptors, Quinazolines - pharmacology, Quinazolines - therapeutic use, Receptor, Epidermal Growth Factor - genetics, Ribose, Survival, Toxicity, Tumors, Tyrosine, Xenografts, Xenotransplantation