Nickel‐Electrocatalytic Decarboxylative Arylation to Access Quaternary Centers**-Reference-Cited by-同舟云学术

Nickel‐Electrocatalytic Decarboxylative Arylation to Access Quaternary Centers**

Published:2024-01-18 Issue:8 Volume:63 Page:
ISSN:1433-7851
Container-title:Angewandte Chemie International Edition
language:en
Short-container-title:Angew Chem Int Ed

Author:

Laudadio Gabriele¹^ORCID,Neigenfind Philipp¹^ORCID,Péter Áron¹,Rubel Camille Z.¹,Emmanuel Megan A.²,Oderinde Martins S.³,Ewing Tamara El‐Hayek¹,Palkowitz Maximilian D.⁴,Sloane Jack L.⁴,Gillman Kevin W.⁴,Ridge Daniel⁴,Mandler Michael D.³,Bolduc Philippe N.⁵,Nicastri Michael C.⁵,Zhang Benxiang¹,Clementson Sebastian⁶,Petersen Nadia Nasser⁶,Martín‐Gago Pablo⁶,Mykhailiuk Pavel⁷⁸,Engle Keary M.¹^ORCID,Baran Phil S.¹^ORCID

Affiliation:

1. Department of Chemistry Scripps Research 10550 North Torrey Pines Road La Jolla CA 92037 USA

2. Chemical Process Development Bristol Myers Squibb 1 Squibb Drive New Brunswick NJ 08901 USA

3. Small Molecule Drug Discovery Bristol Myers Squibb Research & Early Development Route 206 & Province Line Road Princeton NJ 08543 USA

4. Small Molecule Drug Discovery Bristol Myers Squibb Research & Early Development 250 Water Street Cambridge MA 02141 USA

5. Biogen Inc. 225 Binney Street Cambridge MA 02142 USA

6. Research and Early Development, LEO Pharma A/S 2750 Ballerup Denmark

7. Enamine Ltd. Winston Churchill Street 78 02094 Kyiv Ukraine

8. Chemistry Department Taras Shevchenko National University of Kyiv Volodymyrska 64 01601 Kyiv Ukraine

Abstract

AbstractThere is a pressing need, particularly in the field of drug discovery, for general methods that will enable direct coupling of tertiary alkyl fragments to (hetero)aryl halides. Herein a uniquely powerful and simple set of conditions for achieving this transformation with unparalleled generality and chemoselectivity is disclosed. This new protocol is placed in context with other recently reported methods, applied to simplify the routes of known bioactive building blocks molecules, and scaled up in both batch and flow. The role of pyridine additive as well as the mechanism of this reaction are interrogated through Cyclic Voltammetry studies, titration experiments, control reactions with Ni(0) and Ni(II)‐complexes, and ligand optimization data. Those studies indicate that the formation of a BINAPNi(0) is minimized and the formation of an active pyridine‐stabilized Ni(I) species is sustained during the reaction. Our preliminary mechanistic studies ruled out the involvement of Ni(0) species in this electrochemical cross‐coupling, which is mediated by Ni(I) species via a Ni(I)‐Ni(II)‐Ni(III)‐Ni(I) catalytic cycle.

Funder

George E. Hewitt Foundation for Medical Research

H2020 Marie Skłodowska-Curie Actions

National Science Foundation

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/am-pdf/10.1002/anie.202314617

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