Abstract
Cytosine, a DNA and RNA building-block, and Metformin, the most widely prescribed drug for the treatment of Type 2 Diabetes mellitus were made to react separately with ammonium or sodium metavanadates in acidic aqueous solutions to obtain two polyoxovanadate salts with a 6:1 ratio of cation-anion. Thus, compounds [HCyt]6[V10O28]·4H2O, 1 and [HMetf]6[V10O28]·6H2O, 2 (where HCyt = Cytosinium cation, [C4H6N3O]+ and HMetf = Metforminium cation, [C4H12N5]+) were obtained and characterized by elemental analysis, single crystal X-ray diffraction, vibrational spectroscopy (IR and Raman), solution 51V-NMR, thermogravimetric analysis (TGA-DTGA), as well as, theoretical methods. Both compounds crystallized in Pspace group with Z' = 1/2, where the anionic charge of the centrosymmetric ion [V10O28]6− is balanced by six Cytosinium and six Metforminium counterions, respectively. Compound 1 is stabilized by π-π stacking interactions coming from the aromatic rings of HCyt cations, as denoted by close contacts of 3.63 Å. On the other hand, guanidinium moieties from the non-planar HMetf in Compound 2 interact with decavanadate μ2-O atoms via N−H···O hydrogen bonds. The vibrational spectroscopic data of both IR and Raman spectra show that the dominant bands in the 1000-450 cm−1 range are due to the symmetric and asymmetric ν(V−O) vibrational modes. In solution, 51V-NMR experiments of both compounds show that polyoxovanadate species are progressively transformed into the monomeric, dimeric and tetrameric oxovanadates. The thermal stability behavior suggests a similar molecular mechanism regarding the loss of water molecules and the decomposition of the organic counterions. Yet, no changes were observed in the TGA range of 540–580°C due to the stability of the [V10O28]6− fragment. Dispersion-corrected density functional theory (DFT-D) calculations were carried out to model the compounds in aqueous phase using a polarized continuum model calculation. Optimized structures were obtained and the main non-covalent interactions were characterized. Biological activities of these compounds are also under investigation. The combination of two therapeutic agents opens up a window toward the generation of potential metalopharmaceuticals with new and exciting pharmacological properties.
Highlights
Vanadium bioinorganic chemistry is becoming a very important topic in the last decades
Compound [HCyt]6[V10O28]·4H2O, 1, was isolated from an acidic mother solution of NH4VO3 with a pH of around 6, which allowed the protonation of the cytosine molecules and the formation of decavanadate anions
The first attempt to obtain a compound based on [V10O28]6− units and cytosine was initially explored by our group using sodium metavanadate salt NaVO3 as a precursor of polyoxovanadate ions
Summary
Vanadium bioinorganic chemistry is becoming a very important topic in the last decades. The information about vanadium in biological systems is increasing in giant steps, so as a guide for our research we have considered many highlights in the history of the field (See Scheme 1) In this introduction, relevant information will be presented in a limited way. Vanadate(V) solutions can form, under specific conditions, polyoxovanadate species such as the decavanadate anion, [V10O28]6− (Hayashi, 2011) The structure of this oxo-cluster is stable at acidic pH range and structurally contains ten vanadium atoms assembled into a compact structure with unit cell dimensions of 8.3 Å x 7.7 Å x 5.4 Å, where the V5+ metal ions occupy the octahedral interstices in the ten [VO6] units (Swallow and Barnes, 1964; Aureliano, 2011). We combined decavanadate with two biologically relevant molecules Cytosine and Metformin (Scheme 2) with the aim to synthesize compounds with potential pharmacological activity. SCHEME 2 | Molecular diagram of (A) Cytosinium, HCyt and (B) Metforminium, HMetf
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