Abstract
Pharmaceutical salt, nitrofurantoin–4-dimethylaminopyridine (NF-DMAP), along with its native components NF and DMAP are scrutinized by FT-IR and FT-Raman spectroscopy along with density functional theory so that an insight into the H-bond patterns in the respective crystalline lattices can be gained. Two different functionals, B3LYP and wB97X-D, have been used to compare the theoretical results. The FT-IR spectra obtained for NF-DMAP and NF clearly validate the presence of C33–H34⋅⋅⋅O4 and N23–H24⋅⋅⋅N9 hydrogen bonds by shifting in the stretching vibration of –NH and –CH group of DMAP+ towards the lower wavenumber side. To explore the significance of hydrogen bonding, quantum theory of atoms in molecules (QTAIM) has been employed, and the findings suggest that the N23–H24⋅⋅⋅N9 bond is a strong intermolecular hydrogen bond. The decrement in the HOMO-LUMO gap, which is calculated from NF → NF-DMAP, reveals that the active pharmaceutical ingredient is chemically less reactive compared to the salt. The electrophilicity index (ω) profiles for NF and DMAP confirms that NF is acting as electron acceptor while DMAP acts as electron donor. The reactive sites of the salt are plotted by molecular electrostatic potential (MEP) surface and calculated using local reactivity descriptors.
Highlights
The active pharmaceutical ingredient (API) is a drug or a chemical liable for the pharmacological and therapeutic activities in the body
The crystal structure determination of NF-DMAP salt suggests its crystallization in the monoclinic space group P21/c with one molecule each of NF− and DMAP+ in the asymmetric unit [18]
No H-bond interactions are present between one unit of NF-DMAP and other (Figure S3)
Summary
The active pharmaceutical ingredient (API) is a drug or a chemical liable for the pharmacological and therapeutic activities in the body. The market value of a drug can be drastically reduced due to its poor physicochemical properties, which in turn can cause the demand to replace it. This is the major reason why there is an increased interest in the physicochemical properties upgradation methods such as salt formation [3]. Pharmaceutical salts are ionizable drugs that have been combined with a counter-ion to form a neutral compound. The presence of ionizable groups in the molecule is an essential requirement for the formation of salts. An API can be either in the form of cation (approximately 75% of pharmaceutical salts) or anion, and the counter
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