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Abstract
In this study, we investigated differential molecular interactions of crystalline and amorphous
forms of telmisartan (TEL), which is a non-peptide angiotensin-II receptor antagonist
commonly used in the management of hypertension. Amorphous telmisartan (AM-TEL) was
prepared using quench cooling of the melt. The analysis of solid-state properties of AM-TEL
using differential scanning calorimetry (DSC) and X-ray powder diffraction (XRD) confirmed
formation of AM-TEL. Based on a comparative analysis of molecular interactions using spectral
(FTIR and 13C solid-state NMR) and computational tools, we demonstrated that amorphous
telmisartan shows altered molecular interactions. Molecular dynamics simulation of amorphous
and crystalline forms demonstrate that the amorphous form retained some of the molecular
interactions in its disordered molecular arrangement, with a relatively stronger (decrease in bond
length) but lesser (up to only 2.6 % of the population) hydrogen bonding network as compared
with the crystalline counterpart (up to 76% of the population)
