%0 Journal Article %T Development of Novel Benzimidazole Derivates as Potent and Selective Akt Kinase Inhibitors Using <i>In-silico</i> Approaches %A Rasha Ghanem Kattoub %A Faten Sliman %A Mohammad Kousara %J International Journal of Organic Chemistry %P 106-127 %@ 2161-4695 %D 2021 %I Scientific Research Publishing %R 10.4236/ijoc.2021.113009 %X The serine/threonine Akt kinase signaling pathway plays an essential role not only in tumorigenesis but also in the potential response to anticancer therapeutic agents. Therefore, aiming to identify potent and selective Akt inhibitors, a novel series of benzimidazole derivatives were designed and docked within the crystal structure of Akt1 kinase. In order to predict their selectivity, the hit compounds were docked against the protein kinase A (PKA), which is the closely related AGC family kinase protein. Moreover, in-silico ADMET-related descriptors were estimated to predict the pharmacokinetic properties for the selected compounds. Among the designed molecules, four compounds were found to have the best binding affinity and good selectivity to Akt1 kinase, furthermore, those compounds had acceptable ADMET properties and were predicted to be non-mutagenic, which could account them as promising Akt1 inhibitory agents for further investigations. %K Akt %K Selective ATP-competitive Inhibitors %K Benzimidazole %K Molecular Docking %K < %K i> %K In-silico< %K /i> %K ADMET %U http://www.scirp.org/journal/PaperInformation.aspx?PaperID=112125