What does this research mean for the field?

Chemo- and enantioselective hydrosilylation of N-propargyl-indan-1-imines enables the synthesis of enantioenriched N-propargyl-1-indanamines, including (R)-rasagiline, with yields up to 99% and enantioselectivities ranging from 18% to 99% ee. Novelty: ClaimNovelty.METHODOLOGICAL. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The aim is to synthesize (R)-rasagiline and its analogues through an efficient hydrosilylation process.

March 7, 2026

Synthesis of ( R )‐Rasagiline and its Analogues via Chemo‐ and Enantioselective Hydrosilylation of N ‐Propargyl‐indan‐1‐imines

Key Points

The aim is to synthesize (R)-rasagiline and its analogues through an efficient hydrosilylation process.
Utilized a chiral picolinamide Lewis base catalyst derived from chloramphenicol.
Performed chemo- and enantioselective hydrosilylation on N-propargyl-indan-1-imines.
Synthesized various enantioenriched N-propargyl-1-indanamines.
Achieved moderate to good yields of up to 99%.
Obtained enantioselectivities ranging from 18% to 75% ee, with one case reaching 99% ee.

Abstract

ABSTRACT By using a rigid chiral picolinamide Lewis base catalyst prepared from commercially available and cost‐effective chloramphenicol base, chemo‐ and enantioselective hydrosilylation of N ‐propargyl‐indan‐1‐imines has been realized. This transformation allowed the synthesis of various enantioenriched N ‐propargyl‐1‐indanamines including ( R )‐rasagiline with moderate to good yields (up to 99%) in low to good enantioselectivities, typically ranging 18%–75% ee and in one case up to 99% ee.

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Synthesis of ( R )‐Rasagiline and its Analogues via Chemo‐ and Enantioselective Hydrosilylation of N ‐Propargyl‐indan‐1‐imines

Key Points

Abstract

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