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Halogen-Aromatic π Interactions Modulate Inhibitor Residence Times.


ABSTRACT: Prolonged drug residence times may result in longer-lasting drug efficacy, improved pharmacodynamic properties, and "kinetic selectivity" over off-targets with high drug dissociation rates. However, few strategies have been elaborated to rationally modulate drug residence time and thereby to integrate this key property into the drug development process. Herein, we show that the interaction between a halogen moiety on an inhibitor and an aromatic residue in the target protein can significantly increase inhibitor residence time. By using the interaction of the serine/threonine kinase haspin with 5-iodotubercidin (5-iTU) derivatives as a model for an archetypal active-state (type I) kinase-inhibitor binding mode, we demonstrate that inhibitor residence times markedly increase with the size and polarizability of the halogen atom. The halogen-aromatic π interactions in the haspin-inhibitor complexes were characterized by means of kinetic, thermodynamic, and structural measurements along with binding-energy calculations.

SUBMITTER: Heroven C 

PROVIDER: S-EPMC7615044 | biostudies-literature | 2018 Jun

REPOSITORIES: biostudies-literature

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Halogen-Aromatic π Interactions Modulate Inhibitor Residence Times.

Heroven Christina C   Georgi Victoria V   Ganotra Gaurav K GK   Brennan Paul P   Wolfreys Finn F   Wade Rebecca C RC   Fernández-Montalván Amaury E AE   Chaikuad Apirat A   Knapp Stefan S  

Angewandte Chemie (International ed. in English) 20180509 24


Prolonged drug residence times may result in longer-lasting drug efficacy, improved pharmacodynamic properties, and "kinetic selectivity" over off-targets with high drug dissociation rates. However, few strategies have been elaborated to rationally modulate drug residence time and thereby to integrate this key property into the drug development process. Herein, we show that the interaction between a halogen moiety on an inhibitor and an aromatic residue in the target protein can significantly in  ...[more]

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