# Stereoselective Synthesis and Biological Evaluation of Perhydroquinoxaline-Based κ Receptor Agonists

**Authors:** Jonathan Hoffmann, Dirk Schepmann, Constantin Daniliuc, Marcel Bermudez, Bernhard Wünsch

PMC · DOI: 10.3390/ijms26030998 · 2025-01-24

## TL;DR

This paper describes the synthesis and testing of a new compound that selectively activates the κ receptor with high specificity.

## Contribution

A novel perhydroquinoxaline-based κ receptor agonist with high selectivity and structural confirmation via X-ray analysis is presented.

## Key findings

- Compound 14 showed moderate κ receptor affinity (Ki = 599 nM).
- It exhibited high selectivity over μ, δ, σ1, and σ2 receptors.
- X-ray crystal structure analysis confirmed the compound's relative configuration.

## Abstract

The hydroxylated perhydroquinoxaline 14 was designed by conformational restriction of the prototypical κ receptor agonist U-50,488 and the introduction of an additional polar group. The synthesis of 14 comprised ten reaction steps starting from diethyl 3-hydroxyglutarate (4). The first key step was the diastereoselective establishment of the tetrasubstituted cyclohexane 7 by the reaction of dialdehyde 6 with benzylamine and nitromethane. The piperazine ring was annulated by the reaction of silyloxy-substituted cyclohexanetriamine 8 with dimethyl oxalate. The pharmacophoric structural elements characteristic for κ receptor agonists were finally introduced by functional group modifications. The structure including the relative configuration of the tetrasubstituted cyclohexane derivative (2r,5s)-7a and the perhydroquinoxaline 9 was determined unequivocally by X-ray crystal structure analysis. The hydroxylated perhydroquinoxaline 14 showed moderate κ receptor affinity (Ki = 599 nM) and high selectivity over μ, δ, σ1, and σ2 receptors. An ionic interaction between the protonated pyrrolidine of 14 and D138 of κ receptor anchors 14 in the κ receptor binding pocket.

## Linked entities

- **Proteins:** LOC129446843 (olfactory receptor 1468)
- **Chemicals:** U-50,488 (PubChem CID 3036289), diethyl 3-hydroxyglutarate (PubChem CID 96259), benzylamine (PubChem CID 7504), nitromethane (PubChem CID 6375), dimethyl oxalate (PubChem CID 11120)

## Figures

8 figures with captions in the complete paper: https://tomesphere.com/paper/PMC11817610/full.md

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Source: https://tomesphere.com/paper/PMC11817610