Pharmaceutical diversification via palladium oxidative addition complexes.
Mycah R UehlingRyan P KingShane W KrskaTim CernakStephen L BuchwaldPublished in: Science (New York, N.Y.) (2019)
Palladium-catalyzed cross-coupling reactions have transformed the exploration of chemical space in the search for materials, medicines, chemical probes, and other functional molecules. However, cross-coupling of densely functionalized substrates remains a major challenge. We devised an alternative approach using stoichiometric quantities of palladium oxidative addition complexes (OACs) derived from drugs or drug-like aryl halides as substrates. In most cases, cross-coupling reactions using OACs proceed under milder conditions and with higher success than the analogous catalytic reactions. OACs exhibit remarkable stability, maintaining their reactivity after months of benchtop storage under ambient conditions. We demonstrated the utility of OACs in a variety of experiments including automated nanomole-scale couplings between an OAC derived from rivaroxaban and hundreds of diverse nucleophiles, as well as the late-stage derivatization of the natural product k252a.
Keyphrases
- air pollution
- particulate matter
- venous thromboembolism
- atrial fibrillation
- small molecule
- machine learning
- ms ms
- high throughput
- pulmonary embolism
- quantum dots
- emergency department
- high performance liquid chromatography
- drug induced
- gas chromatography mass spectrometry
- fluorescence imaging
- molecularly imprinted
- tandem mass spectrometry
- solid phase extraction
- gas chromatography
- electronic health record