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Rational drug redesign to overcome drug resistance in cancer therapy: imatinib moving target.

ABSTRACT: Protein kinases are central targets for drug-based cancer treatment. To avoid functional impairment, the cell develops mechanisms of drug resistance, primarily based on adaptive mutations. Redesigning a drug to target a drug-resistant mutant kinase constitutes a therapeutic challenge. We approach the problem by redesigning the anticancer drug imatinib guided by local changes in interfacial de-wetting propensities of the C-Kit kinase target introduced by an imatinib-resistant mutation. The ligand is redesigned by sculpting the shifting hydration patterns of the target. The association with the modified ligand overcomes the mutation-driven destabilization of the induced fit. Consequently, the redesigned drug inhibits both mutant and wild-type kinase. The modeling effort is validated through molecular dynamics, test tube kinetic assays of downstream phosphorylation activity, high-throughput bacteriophage-display kinase screening, cellular proliferation assays, and cellular immunoblots. The inhibitor redesign reported delineates a molecular engineering paradigm to impair routes for drug resistance.

SUBMITTER: Fernandez A 

PROVIDER: S-EPMC2769247 | biostudies-literature | 2007 May

REPOSITORIES: biostudies-literature

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Rational drug redesign to overcome drug resistance in cancer therapy: imatinib moving target.

Fernández Ariel A   Sanguino Angela A   Peng Zhenghong Z   Crespo Alejandro A   Ozturk Eylem E   Zhang Xi X   Wang Shimei S   Bornmann William W   Lopez-Berestein Gabriel G  

Cancer research 20070501 9

Protein kinases are central targets for drug-based cancer treatment. To avoid functional impairment, the cell develops mechanisms of drug resistance, primarily based on adaptive mutations. Redesigning a drug to target a drug-resistant mutant kinase constitutes a therapeutic challenge. We approach the problem by redesigning the anticancer drug imatinib guided by local changes in interfacial de-wetting propensities of the C-Kit kinase target introduced by an imatinib-resistant mutation. The ligand  ...[more]

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