Biophysical and Biochemical Characterization of Structurally Diverse Small Molecules Hits for KRAS Inhibition

Biophysical and Biochemical Characterization of Structurally Diverse Small Molecules Hits for KRAS Inhibition

We describe six compounds as early hits for the development of direct inhibitors of KRAS, an important anticancer drug target. We show that these compounds bind to KRAS with affinities in the low micromolar range and exert different effects on its interactions with binding partners. Some of the comp...

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Veröffentlicht in:Chembiochem : a European journal of chemical biology 2024-02, p.e202300827
Hauptverfasser: Pagba, Cynthia, Gupta, Amit K, Dilsha, Kasuni, Sadrpour, Parisa, Jakubec, Jacob, Prakash, Priyanka, van der Hoeven, Dharini, Cho, Kwang-Jin, Gilbertson, Scott, Gorfe, Alemayehu A
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creator Pagba, Cynthia
Gupta, Amit K
Dilsha, Kasuni
Sadrpour, Parisa
Jakubec, Jacob
Prakash, Priyanka
van der Hoeven, Dharini
Cho, Kwang-Jin
Gilbertson, Scott
Gorfe, Alemayehu A
description We describe six compounds as early hits for the development of direct inhibitors of KRAS, an important anticancer drug target. We show that these compounds bind to KRAS with affinities in the low micromolar range and exert different effects on its interactions with binding partners. Some of the compounds exhibit selective binding to the activated form of KRAS and inhibit signal transduction through both the MAPK or the phosphatidylinositide 3-kinase PI3K-protein kinase B (AKT) pathway in cells expressing mutant KRAS. Most inhibit intrinsic and/or SOS-mediated KRAS activation while others inhibit RAS-effector interaction. We propose these compounds as starting points for the development of non-covalent allosteric KRAS inhibitors.
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title Biophysical and Biochemical Characterization of Structurally Diverse Small Molecules Hits for KRAS Inhibition
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