Diversity of Solid Forms Promoted by Ball Milling: Characterization and Intrinsic Dissolution Studies of Pioglitazone Hydrochloride and Fluvastatin Sodium Drug-Drug Systems

Marco Villeda-Villegas; José C Páez-Franco; Guadalupe Coyote-Dotor; Alejandra Núñez-Pineda; Alejandro Dorazco-González; Inés Fuentes-Noriega; Kenneth Rubio-Carrasco; Helen P Toledo Jaldín; David Morales-Morales; Juan Manuel Germán-Acacio

doi:10.3390/ph16060781

Diversity of Solid Forms Promoted by Ball Milling: Characterization and Intrinsic Dissolution Studies of Pioglitazone Hydrochloride and Fluvastatin Sodium Drug-Drug Systems

Pharmaceuticals (Basel). 2023 May 24;16(6):781. doi: 10.3390/ph16060781.

Affiliations

¹ Red de Apoyo a la Investigación, Coordinación de la Investigación Científica-UNAM, Instituto Nacional de Ciencias Médicas y Nutrición SZ, Ciudad de Mexico 14000, Mexico.
² Centro Conjunto de Investigación en Química Sustentable CCIQS UAEM-UNAM Carretera Toluca-Atlacomulco km 14.5, Toluca 50200, Mexico.
³ Instituto de Química, Universidad Nacional Autónoma de Mexico, Circuito Exterior, Ciudad Universitaria, Ciudad de Mexico 04510, Mexico.
⁴ Laboratorio de Biofarmacia, Departamento de Farmacia, Facultad de Química-UNAM, Ciudad de México 04510, Mexico.
⁵ Technological Superior Studies Tianguistenco, Mechanical Engineering, Santiago Tianguistenco 52650, Mexico.

Abstract

Coamorphous salt in a 1:1 ratio prepared by ball milling from Fluvastatin sodium (FLV) and Pioglitazone hydrochloride (PGZ·HCl) can be selectively formed by neat grinding (NG). Furthermore, the salt-cocrystal continuum was preferably formed by employing liquid-assisted grinding (LAG) using ethanol (EtOH). Attempts to prepare the coamorphous salt starting from the salt-cocrystal continuum by NG were unsuccessful. Interestingly, through ball milling by NG or LAG, a great diversity of solid forms (PGZ·HCl-FLV 1:1) could be accessed: NG and hexane (coamorphous); ethyl acetate (physical mixture); EtOH (salt-cocrystal continuum); and water (which presents two T_g, indicating immiscibility of the components). An exploration was performed at different drug-to-drug ratios by NG. By differential scanning calorimetry (DSC), the presence of two endothermic events was observed in this screening: incongruous melting point (solidus) and excess of one of the components (liquidus), except in the 1:1 solid form. From these results, eutectic behavior was observed. Through the construction of a binary phase diagram, it was determined that the 1:1 molar ratio gives rise to the formation of the most stable coamorphous composition. Dissolution profile studies of these solid forms were carried out, specifically on pure FLV and the solid forms of PGZ⋅HCl-FLV (1:2; 1:4; and 1:6), together with the coamorphous 1:1 salt. By itself, pure FLV presented the highest K_int (13.6270 ± 0.8127 mg/cm²⋅min). On the other hand, the coamorphous 1:1 showed a very low K_int (0.0220 ± 0.0014 mg/cm²·min), indicating very fast recrystallization by the FLV, which avoids observing a sudden release of this drug in the solution. This same behavior was observed in the eutectic composition 1:2. In the other solid forms, the value of K_int increases along with the %w of FLV. From the mechanochemical point of view, ball milling by NG or LAG became an important synthetic tool since it allows obtaining a great variety of solid forms to explore the solid-state reactivity of the drug-drug solid-form PGZ HCl-FLV.

Keywords: XPS experiments; drug–drug coamorphous; drug–drug salt–cocrystal continuum; fluvastatin sodium; intrinsic dissolution experiments; mechanochemical reactions; pioglitazone hydrochloride.

Grants and funding

IT200920/PAPIIT-DGAPA-UNAM