Synthesis, anti-proliferative activity, SAR study, and preliminary in vivo toxicity study of substituted N,N’-bis(arylmethyl)benzimidazolium salts against a panel of non-small cell lung cancer cell lines

Publication date: Available online 5 November 2016
Source:Bioorganic & Medicinal Chemistry
Author(s): Kerri L. Shelton, Michael A. DeBord, Patrick O. Wagers, Marie R. Southerland, Travis M. Williams, Nikki K. Robishaw, Leah P. Shriver, Claire A. Tessier, Matthew J. Panzner, Wiley J. Youngs
A series of N,N'-bis(arylmethyl)benzimidazolium salts have been synthesized and evaluated for their in vitro anti-cancer activity against select non-small cell lung cancer cell lines to create a structure activity relationship profile. The results indicate that hydrophobic substituents on the salts increase the overall anti-proliferative activity. Our data confirms that naphthylmethyl substituents at the nitrogen atoms (N¹(N³)) and highly lipophilic substituents at the carbon atoms (C² and C⁵(C⁶)) can generate benzimidazolium salts with anti-proliferative activity that is comparable to that of cisplatin. The National Cancer Institute's Developmental Therapeutics Program tested 1, 3-5, 10, 11, 13-18, 20-25, and 28-30 in their 60 human tumor cell line screen. Results were supportive of data observed in our lab. Compounds with hydrophobic substituents have higher anti-cancer activity than compounds with hydrophilic substituents.

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