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Aromatic–aromatic interaction of amitriptyline: Implication of overdosed drug detoxification

✍ Scribed by Dong-Won Lee; Jason Flint; Timothy Morey; Donn Dennis; Richard Partch; Ronald Baney

Publisher: John Wiley and Sons
Year: 2005
Tongue: English
Weight: 136 KB
Volume: 94
Category: Article
ISSN: 0022-3549
DOI: 10.1002/jps.20256

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✦ Synopsis

The objectives of this work are to explore the p-p complexation of amitriptyline with p electron-deficient aromatic rings and demonstrate the feasibility of p-p complexation for overdosed drug detoxification. Water-soluble oligochitosan was chemically modified with dinitrobenzenesulfonyl groups to induce selective binding toward amitriptyline through p-p complexation. NMR studies showed that benzenesulfonyl and dinitrobenzenesulfonyl protons were upfield shifted by the addition of amitriptyline, indicating the formation of p-p complexes. The p-p complexation of amitriptyline is driven primarily by a desolvation driving force, whereas the magnitude of interaction is dictated by the complementrary electrostatic interaction. Isolated rat heart tests revealed that dinitrobenzenesulfonyl oligochitosan prevented the amitriptylineinduced cardiotoxicity and was itself not cardiotoxic.

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