What question did this study set out to answer?

The aim is to develop a scalable and efficient synthesis method for the nonsteroidal antagonist (S)-finerenone.

March 2, 2026

Synthesis of ( S )-Finerenone via Late-Stage Asymmetric Transfer Hydrogenation

Key Points

The aim is to develop a scalable and efficient synthesis method for the nonsteroidal antagonist (S)-finerenone.
Designed a convergent synthesis strategy for (S)-finerenone.
Utilized a chromatography-free approach achieving 88% yield of racemic precursor.
Implemented dynamic kinetic resolution (DKR) using chiral phosphoric acid for asymmetric transfer hydrogenation.
Achieved a high overall yield of 88% for the racemic precursor.
Developed two complementary methods for synthesis, enhancing enantioselectivity.
Provided an efficient resolution process utilizing (+)-benzoyl tartaric acid.

Abstract

Herein, we report a convergent and practical synthesis of the nonsteroidal mineralocorticoid receptor antagonist (S)-finerenone. The present approach incorporates a scalable, chromatography-free method to attain a racemic precursor with an impressive overall yield of 88%. Leveraging this versatile intermediate, we have developed two complementary approaches, including a robust resolution utilizing (+)-benzoyl tartaric acid and an efficient asymmetric transfer hydrogenation facilitated by chiral phosphoric acid-catalyzed dynamic kinetic resolution (DKR), to avoid cumbersome purification procedures, thereby offering a flexible, high-yielding, and highly enantioselective platform for the industrial-scale production of (S)-finerenone.

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Synthesis of ( S )-Finerenone via Late-Stage Asymmetric Transfer Hydrogenation

Key Points

Abstract

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