| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1374464 | Bioorganic & Medicinal Chemistry Letters | 2009 | 4 Pages |
Abstract
A series of C3 halobenzyl-substituted tricyclic HIV integrase inhibitors was prepared. Improvement in cell-based inhibitor potency was observed in comparison to previously disclosed tricyclic pyrroloquinolines carrying the ‘halobenzyl tail’ at the lactam nitrogen. Animal PK for several of the C3-substituted inhibitors was examined, with a dihaloaryl analog achieving good balance in protein-shifted EC50 and t1/2 in animal PK studies.
A series of C3-halobenzyl-substituted tricyclic integrase inhibitors was prepared. Excellent cell-based inhibitor potency was observed, and selected leads in this new series showed good bioavailability and long t1/2 in animal PK studies.Figure optionsDownload full-size imageDownload as PowerPoint slide
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Authors
Sammy Metobo, Michael Mish, Haolun Jin, Salman Jabri, Rachael Lansdown, Xiaowu Chen, Manuel Tsiang, Matthew Wright, Choung U. Kim,