What question did this study set out to answer?

The research aims to develop a new method for enantioselective aminoalkylation using nickel-photoredox catalysis.

March 16, 2026

Nickel/Photoredox-Catalyzed Enantioselective α-Aminoalkylation of 2-Iodopyridines

Key Points

The research aims to develop a new method for enantioselective aminoalkylation using nickel-photoredox catalysis.
Utilized chiral Ni-PHOX complexes and photoredox catalysis for asymmetric coupling.
Applied the reaction to 2-iodopyridines at the C2-position.
Conducted computational studies and DFT analysis to explore the mechanism and selectivity.
Achieved enantioselective synthesis of chiral pyrid-2-yl β-aminoalcohols.
Methodology proved effective for other heteroarenes like quinolines and azines.
Demonstrated scalability of the reaction up to one gram.

Abstract

Chiral Ni-PHOX complexes in combination with photoredox catalysis are shown to be effective to achieve the asymmetric coupling of amino acids with 2-iodopyridines at the C2-position. The regio- and enantioselective protocol developed herein enables direct access to chiral pyrid-2-yl β-aminoalcohols, which are found in many active pharmaceutical ingredients. This methodology can be extended to other heteroarenes, such as quinolines and azines, on one gram scale. Computational studies supported by experimentation revealed the trend of ligand steric and electronic influences on enantioselectivity. A plausible mechanism was proposed using DFT to further rationalize the observed regio- and enantioselectivity.

Bookmark

Nickel/Photoredox-Catalyzed Enantioselective α-Aminoalkylation of 2-Iodopyridines

Key Points

Abstract

Cite This Study