| Literature DB >> 25973297 |
Thomas W Grunt1, Alexandra Hebar2, Sylvia Laffer3, Renate Wagner4, Barbara Peter5, Harald Herrmann5, Alexandra Graf6, Martin Bilban7, Martin Posch6, Gregor Hoermann7, Matthias Mayerhofer7, Gregor Eisenwort3, Christoph C Zielinski1, Edgar Selzer2, Peter Valent5.
Abstract
Advanced colorectal cancer is characterized by uncontrolled growth and resistance against anti-cancer agents, including ErbB inhibitors. Recent data suggest that cancer stem cells (CSC) are particularly resistant. These cells may reside within a CD133+ fraction of the malignant cells. Using HCT116 cells we explored the role of CD133 and other CSC markers in drug resistance in colon cancer cells. CD133+ cells outnumbered CD133- cells over time in long-term culture. Both populations displayed the KRAS mutation 38G > A and an almost identical target profile, including EGFR/ErbB1, ErbB2, and ErbB4. Microarray analyses and flow cytometry identified CD26 as additional CSC marker co-expressed on CD133+ cells. However, knock-down of CD133 or CD26 did not affect short-term growth of HCT116 cells, and both cell-populations were equally resistant to various targeted drugs except irreversible ErbB inhibitors, which blocked growth and ERK1/2 phosphorylation in CD133- cells more efficiently than in CD133+ cells. Moreover, the MEK inhibitor AS703026 was found to overcome resistance against ErbB blockers in CD133+ cells. Together, CD133 and CD26 are markers of long-term growth and resistance to ErbB blockers in HCT116 cells, which may be mediated by constitutive ERK activity.Entities:
Keywords: CD133; CD26; Cancer stem cell; DPPIV; EGFR/ErbB; HCT116; colon cancer; drug resistance
Year: 2015 PMID: 25973297 PMCID: PMC4396035
Source DB: PubMed Journal: Am J Cancer Res ISSN: 2156-6976 Impact factor: 6.166