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Cancer stem cell drugs target K-ras signaling in a stemness context.

Oncogene.. 2016-10; 
Najumudeen AK, Jaiswal A, Lectez B, Oetken-Lindholm C, Guzmán C, Siljamäki E, Posada IM, Lacey E, Aittokallio T, Abankwa D.
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Plasmid DNA Preparation ... Plasmid pcDNA3.1+N-HA with wild-type human Calmodulin1 (NM 006888) (wild-type-CaM) and mutant CaM plasmid (mut-CaM) with substitutions K75Q, K77Q and K148Q were generated by GenScript USA Inc. (Piscataway, NJ, USA). ... Get A Quote

摘要

Cancer stem cells (CSCs) are considered to be responsible for treatment relapse and have therefore become a major target in cancer research. Salinomycin is the most established CSC inhibitor. However, its primary mechanistic target is still unclear, impeding the discovery of compounds with similar anti-CSC activity. Here, we show that salinomycin very specifically interferes with the activity of K-ras4B, but not H-ras, by disrupting its nanoscale membrane organization. We found that caveolae negatively regulate the sensitivity to this drug. On the basis of this novel mechanistic insight, we defined a K-ras-associated and stem cell-derived gene expression signature that predicts the drug response of cancer cells... More

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