Palladium‐Catalyzed PIDA‐Mediated δ‐C(sp3)−H Acetoxylation of Amino Acid Derivatives: Overriding Competitive Intramolecular Amination

The selective δ‐C(sp3)−H acetoxylation of N‐(SO2Py)‐protected amino acid derivatives has been accomplished by using palladium‐catalysis and PhI(OAc)2 (PIDA) as both terminal oxidant and acetoxy source. The distinct structural and electronic features of the SO2Py compared to more traditional carbonyl...

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Bibliographic Details
Published in:Angewandte Chemie 2022-11, Vol.134 (47), p.n/a
Main Authors: Martínez‐Mingo, Mario, García‐Viada, Andrés, Prendes, Daniel Sowa, Alonso, Inés, Rodríguez, Nuria, Arrayás, Ramón Gómez, Carretero, Juan C.
Format: Article
Language:English
Subjects:
Acetoxylation
Amination
Amino Acids
Carbonyl compounds
Carbonyls
Catalysis
Chemistry
Directing Groups
Oxidants
Oxidizing agents
Palladium
Palladium Catalysis
Regioselectivity
Remote C−H Activation
Selectivity
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Summary:The selective δ‐C(sp3)−H acetoxylation of N‐(SO2Py)‐protected amino acid derivatives has been accomplished by using palladium‐catalysis and PhI(OAc)2 (PIDA) as both terminal oxidant and acetoxy source. The distinct structural and electronic features of the SO2Py compared to more traditional carbonyl‐based directing groups is essential to override the otherwise more favourable competitive intramolecular C−H amination. The δ‐site selectivity predominates over traditionally more favorable 5‐membered cyclopalladation at competitive γ‐CH2. Experimental and DFT mechanistic studies provide important insights about the mechanism and the underlying factors controlling the chemo‐ and regioselectivity. Selective δ‐C(sp3)−H acetoxylation of amino acid derivatives has been achieved by using palladium‐catalysis and PhI(OAc)2 (PIDA) as terminal oxidant and acetoxy source. The N‐SO2Py protecting/directing group plays a key role in enabling control of chemoselectivity (intermolecular C−O over intramolecular C−N bond formation) and regioselectivity (favoring δ‐CH3 over γ‐CH2 activation).
ISSN:0044-8249
1521-3757
DOI:10.1002/ange.202209865