Mechanochemistry synthesis was applied
to the supramolecular synthesis
and green scale-up production of a 1:1 drug–drug cocrystal
involving the antimetabolite prodrug 5-Fluorocytosine (5-FC) and the
tuberculostatic drug Isoniazid (INH), namely, 5FC-INH. Crystalline
material, also obtained by traditional slow evaporation methods, was
analyzed by single-crystal X-ray diffraction (XRD). The crystal packing
is stabilized by a classical N–H···N hydrogen-bond
interaction between the amine moiety of 5-FC and the INH pyridine
nitrogen. IR and Raman data provided spectroscopic evidence about
the hydrogen atom positions, thereby confirming the neutral nature
of the cocrystal. Furthermore, 5FC-INH codrug was also evaluated by
a range of analytical techniques such as powder XRD and thermal (thermogravimetric
analysis, differential scanning calorimetry, hot stage microscopy)
analyses. A physical stability study was performed in high relative
humidity conditions to verify possible 5-FC solid-state hydration
and/or INH degradation. The equilibrium solubility of this codrug
was compared to the anhydrous 5-FC and INH raw materials, in pH 1.2
buffer media, and it was found to be similar to that of 5-FC, a biopharmaceutics
classification system class I drug. The results show that the cocrystal
has superior phase stability properties against moisture when compared
to the starting pharmaceutical ingredients, so it could be considered
as a potential candidate for the treatment of concomitant fungal infections,
tuberculosis, and cancer.
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