Theoretical investigations on R(O)nS-NO (n=0,1,2) systems

In the current article we report the ab initio study on the stability of S-Nitrosothiols (MeSNO, 1) and their oxidised derivatives (MeS(O)NO, 2) and (MeS(O)₂NO, 3). The bond length, bond order, rotational barrier and bond dissociation energy have been calculated and compared with that of sulfenamide (HS-NH₂) and its oxidised derivatives sulfinamide (H(O)S-NH₂) and sulfonamide (H(O)₂S-NH₂). The S-N bond dissociation energy in the oxidised state is very small compared to parent RSNO indicating the weakness of sigma bond. NBO analysis suggests that the negative hyperconjugative interactions are very strong in S-nitrosothiols and their oxidised derivatives, which weaken the sigma bond and facilitate the release of nitric oxide.     

Electronic structure of N-sulfonylimines

The electronic structure of N-sulfonylimines has been studied in detail using ab initio MO and density functional methods. The S–N rotational barriers in HS(O)₂N=CH₂ at G2MP2 and CBS-Q levels have been found to be 3.25 and 3.43 kcal/mol respectively. Complete optimization at HF/6-31+G^*, MP2(full)/6-31+G^* and B3LYP/6-31+G^* levels have shown that synperiplanar arrangement of S–O with respect to C=N is more stable. NBO analysis has been carried out to quantitatively estimate these delocalisations and charge polarization in RS(O)₂N=CH₂ (R=H, Me, Cl, F). The Lewis basic character in N-sulfonylimines is less compared to N-alkylimines due to anomeric interactions that reduce the lone pair electron density on nitrogen in 1.     

Electron deficient bridges involving silylenes: a theoretical study

Ab initio and density functional studies show that silylenes can form complexes with BH(3) and the resultant complexes possess 3c-2e bridges. The complexation energy for the formation of the these H-bridged structures is in the range of 18-46 kcal/mol. The characteristics of the electron deficient bridges depend on the substituents attached to the silylenes. With an increase in the pi-donating capacity of the substituents, the exothermicity of complex formation gets reduced but the kinetic stability of the H-bridged structures increase. The natural bond orbital analysis shows that all the H-bridged structures are associated with sigma(B-H)-->ppi(Si) second-order delocalization, which is responsible for the origin of the 3c-2e bonds. The complexation energies of the silylene-BH(3) complexes have been shown to have a correlation to the singlet-triplet energy gaps of silylenes.     

Polymorphs and Polymorphic Cocrystals of Temozolomide

Crystal polymorphism in the antitumor drug temozolomide (TMZ), cocrystals of TMZ with 4,4′‐bipyridine‐N,N′‐dioxide (BPNO), and solid‐state stability were studied. Apart from a known X‐ray crystal structure of TMZ (form 1), two new crystalline modifications, forms 2 and 3, were obtained during attempted cocrystallization with carbamazepine and 3‐hydroxypyridine‐N‐oxide. Conformers A and B of the drug molecule are stabilized by intramolecular amide N? H???N_imidazole and N? H???N_tetrazine interactions. The stable conformer A is present in forms 1 and 2, whereas both conformers crystallized in form 3. Preparation of polymorphic cocrystals I and II (TMZ?BPNO 1:0.5 and 2:1) were optimized by using solution crystallization and grinding methods. The metastable nature of polymorph 2 and cocrystal II is ascribed to unused hydrogen‐bond donors/acceptors in the crystal structure. The intramolecularly bonded amide N–H donor in the less stable structure makes additional intermolecular bonds with the tetrazine C?O group and the imidazole N atom in stable polymorph 1 and cocrystal I, respectively. All available hydrogen‐bond donors and acceptors are used to make intermolecular hydrogen bonds in the stable crystalline form. Synthon polymorphism and crystal stability are discussed in terms of hydrogen‐bond reorganization.     

Tautomeric preferences and electron delocalization in biurets,thiobiurets, and dithiobiurets: An ab initio study

In several literature reports biuret and its sulfur analogs are reported to exist in their diketo form with general formula H₂N? CX? NH? CY? NH₂ (X = O, Y = O, biuret; X = Y = S, dithiobiuret; and X = O, Y = S, thiobiuret). On the other hand, recently reported results on the electronic structure of biguanide analogs (X = Y = NH)demonstrated that a form equivalent to diketo is not the preferred structure. Thus, a systematic ab initio study on the tautomeric preferences of biuret and its sulfur analogs (dithiobiuret and thiobiuret) has been carried out. The results indicate that an interplay of conjugative stabilization and intramolecular hydrogen bonding to play a role in tautomeric preferences. Energy and geometric parameters, natural bond orbital analyses have been employed to understand the chemistry of the title compounds. The results indicate that unlike biguanides, these compounds prefer diketo forms containing hydrogen on the bridging nitrogen (N4) and in a trans‐arrangement (1a–4a). However, tautomerization of these keto forms to the corresponding enol isomers was also found to be highly probable. © 2008 Wiley Periodicals, Inc. Int J Quantum Chem, 2008     

Paclitaxel loaded poly (DL lactic acid co castor oil) 60:40 with poloxamer‐F68 rod shape cylindrical nanoparticle preparation and in vitro cytotoxicity studies

This research presents a thin‐film hydration‐solvent evaporation method to formulate the paclitaxel loaded poly (DL lactic acid co castor oil) 4:6 with poloxamer‐F68 cylindrical shape nanoparticles. The particles were less than 250 nanometers (nm) in size, with an average width of 60 nm and an average length of 100 nm. The percent yield, encapsulation efficiency (EE), and percent drug loading (DL) were detected. This approach produces drug loading values between 5% and 20% w/w. X‐ray powder diffraction (XRD) identified the physicochemical properties of nanoparticles differential scanning calorimetry (DSC) and Fourier‐transform infrared spectroscopy (FTIR). The investigation shows that the drug is molecularly dispersed in polymers or given in an amorphous or semicrystalline state. Horizontal water bath shaker technology considered the in vitro release of PTX loaded nanoparticles under sink conditions. Poly (DL lactic acid co castor oil) 4:6 nanoparticles exhibited a sustained release analysis. At the end of 30 hours, the percent cumulative drug release from the formulations was between 74.52% and 92.87% for F1 and F4. In vitro cytotoxicity assays indicate that PTX having p (DLLA:CO60:40) nanoparticles have a higher cytotoxic effect on MCF‐7/ADR.     

Expanding the conformational pool of cis-beta-sugar amino acid: accommodation of beta-hGly motif in robust 14-helix

Tendencies of forming stable helices of heterooligomers composed of alternating rigid cis-beta-sugar amino acid and flexible beta-hGly motifs have been investigated, using a combination of molecular mechanics, CD, FT-IR, and NMR techniques. The results show that the solution structures of these oligomers exist as robust right-handed 14-helices. Here, we examine the role of conformationally rigid cis-beta-sugar amino acid in preorganizing the conformation of beta-hGly to form the 14-helix. Our findings also show that a right-handed 14-helix can be formed with as few as four properly sequenced heterogeneous residues. These results represent the expansion of the conformational pool of sugar amino acid in the design of well-folded 14-helices, which can be used to develop beta-peptides endowed with biological activity.     

DMAP catalysed vinylogous Rauhut–Currier reaction of allenoates with para-quinone methides

The hitherto unknown, organocatalysed (DMAP) vinylogous Rauhut-Currier reaction of 2,3-butadienoates with para-quinone methides has been achieved. The products, diarylmethane substituted allenoates, are formed in high to excellent yields under mild reaction conditions.     

A green protocol for one pot synthesis of benzosuberone tethered thiadiazolopyrimidine-6-carboxylates using PEG-400 as potent anti-proliferative agents

A new concise and facile method was explored to synthesize a collection of new benzosuberone based thiadiazolo [3,2-a] pyrimidine-6-carboxylates using polyethylene glycol (PEG), which could be regarded as the derivatives of the hybrid scaffolds of bioactive natural benzosuberone and heterocyclic thiadiazolo[3,2-a]pyrimidine. The structures of the synthesized compounds were characterized by ¹H, ¹³C NMR, MS and IR; and their anti-proliferative activity was evaluated against four human cancer cell lines; A549, SKNSH, HeLa and MCF-7. Among the tested compounds, compound 8k showed the most prominent activity against all the cell lines and these results may lay the foundation for further design of novel anti-proliferative agents.     

Convective heat-transfer rate distributions over a missile shaped body flying at hypersonic speeds

Experiments are carried out with air as the test gas to obtain the surface convective heating rate on a missile shaped body flying at hypersonic speeds. The effect of fins on the surface heating rates of missile frustum is also investigated. The tests are performed in a hypersonic shock tunnel at stagnation enthalpy of 2 MJ/kg and zero degree angle of attack. The experiments are conducted at flow Mach number of 5.75 and 8 with an effective test time of 1 ms. The measured stagnation-point heat-transfer data compares well with the theoretical value estimated using Fay and Riddell expression. The measured heat-transfer rate with fin configuration is slightly higher than that of model without fin. The normalized values of experimentally measured heat transfer rate and Stanton number compare well with the numerically estimated results.