Design and Synthesis of Tetrahydropyridothieno[2,3-<i>d</i>]pyrimidine Scaffold Based Epidermal Growth Factor Receptor (EGFR) Kinase Inhibitors: The Role of Side Chain Chirality and Michael Acceptor Group for Maximal Potency - Concepedia

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Design and Synthesis of Tetrahydropyridothieno[2,3-<i>d</i>]pyrimidine Scaffold Based Epidermal Growth Factor Receptor (EGFR) Kinase Inhibitors: The Role of Side Chain Chirality and Michael Acceptor Group for Maximal Potency

DOI Full Paper Access

109

Citations

13

References

2010

Year

Chia-Hsien Wu, Mohane Selvaraj Coumar, Chang-Ying Chu, Wen‐Hsing Lin, Yi‐Rong Chen, Chiung-Tong Chen, Hui-Yi Shiao, Shaik Rafi, Sing-Yi Wang, Hui Hsu,

Journal of Medicinal Chemistry

Kinase InhibitorsMolecular BiologySide Chain ChiralityMaximal PotencyPharmaceutical ChemistryTumor BiologyMedicinal ChemistryHybrid Design StrategyAnti-cancer AgentEgfr KinaseNovel TherapyCancer ResearchTumor TargetingDrug DevelopmentPharmacologyCell BiologyTumor MicroenvironmentNatural SciencesRational Drug DesignMedicineCancer GrowthDrug DiscoveryChiral Side Chain

Abstract

HTS hit 7 was modified through hybrid design strategy to introduce a chiral side chain followed by introduction of Michael acceptor group to obtain potent EGFR kinase inhibitors 11 and 19. Both 11 and 19 showed over 3 orders of magnitude enhanced HCC827 antiproliferative activity compared to HTS hit 7 and also inhibited gefitinib-resistant double mutant (DM, T790M/L858R) EGFR kinase at nanomolar concentration. Moreover, treatment with 19 shrinked tumor in nude mice xenograft model.

References

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