# Double Salts and Racemate in Mefloquine–Ibuprofen and Mefloquine–Ketoprofen Systems. A Structural and Thermochemical Analysis

**Authors:** Juliana B. Martins, João V. Segatto, Juan C. Tenorio, Paulo S. Carvalho

PMC · DOI: 10.1002/chir.70088 · 2026-02-13

## TL;DR

This study explores how combining mefloquine with ibuprofen or ketoprofen forms double salts and racemates, revealing structural and solubility patterns that help understand chiral drug crystallization.

## Contribution

The study demonstrates structural mimicry between double salts and racemates in chiral drug combinations, offering new insights into predictable enantiomeric resolution.

## Key findings

- Double salts and racemates formed with mefloquine show structural similarities to their racemic forms.
- Ketoprofen systems produced isostructural double salts and racemates, while ibuprofen systems had different architectures.
- Solubility and stability varied, with the ketoprofen racemate and ibuprofen double salt being the most soluble.

## Abstract

The formation of salts remains a highly sought‐after yet unpredictable strategy for resolving chiral drugs. Using a drug–drug approach, we have investigated the crystallization behavior of Mefloquine (Mf), a racemic antimalarial drug, in combination with enantiopure (S)‐ibuprofen and (S)‐ketoprofen, as well as their racemic forms. Double salts and racemates have been obtained and characterized by single‐crystal and powder X‐ray diffraction, Hirshfeld surface analysis, thermal analysis (DSC and TGA), and solubility measurements. Structural analysis reveals that the formation of double salts often follows a pattern similar to the packing and supramolecular motifs found in the corresponding racemates. For the ketoprofen systems, the double salt and racemate have been found to be isostructural and isomorphic, whereas the ibuprofen systems display different architectures despite similar unit cells. Both double salts exhibited thermal stability and solubility profiles comparable to their racemic counterparts. On the other hand, the racemate with ketoprofen and the double salt with ibuprofen are the most soluble structures, suggesting that they are more stable systems than their counterparts. These findings support the view that double salt formation in such systems results from structural mimicry of racemates, emphasizing the challenges of predictable enantiomeric resolution and the importance of understanding structure–property relationships in chiral crystallization.

(S)‐ibuprofen or ketoprofen were used to resolve mefloquine, forming double salts structurally similar to the racemic forms.

## Linked entities

- **Chemicals:** Mefloquine (PubChem CID 4046), (S)-ibuprofen (PubChem CID 39912), (S)-ketoprofen (PubChem CID 667550)

## Full-text entities

- **Chemicals:** Mefloquine (MESH:D015767), Salts (MESH:D012492), (S)-ibuprofen (MESH:D007052), (S)-ketoprofen (MESH:D007660)

## Figures

9 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12903187/full.md

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Source: https://tomesphere.com/paper/PMC12903187