Studies on 3,5-diaminopyrazole derivatives

The behaviour of 3,5-diamino-4-phenylazopyrazole toward a variety of reagents is reported. Several new 3,5-diaminopyrazole derivatives as well as amino derivatives of fused pyrazoles have been prepared.

---

Untersuchungen an 3,5-Diaminopyrazol-Derivaten

Zusammenfassung Es wird über das Verhalten von 3,5-Diamino-4-phenylazopyrazol gegenüber verschiedenen Agentien berichtet. Es wurden sowohl einige neue 3,5-Diaminooyrazol-Derivate als auch einige Aminoderivate von kondensierten Pyrazolen dargestellt.

     

Vibrational spectroscopic study on some Hofmann type clathrates: M(2-(1-cyclohexenyl)ethylamine)2Ni(CN)4·2benzene (M=Ni and Cd)

New Hofmann type benzene clathrates in the form of M(CyHEA)2Ni(CN)4·2benzene (where CyHEA=2-(1-cyclohexenyl)ethylamine and M=Ni or Cd) have been prepared in powder form and FT-IR and Raman spectra have been reported. The results suggest that title compounds are similar in structure to Hofmann type clathrates and their structures consist of polymeric layers of |M-Ni(CN)4|∞ with the CyHEA molecule bounded to the metal atoms (M).     

Vibrational spectroscopic study on some Hofmann-Td type clathrates: Ni(4-phenylpyridine)2M(CN)4·2G (M=Cd or Hg, G=1,4-dioxane)

New Hofmann-T(d) type clathrates in the form of Ni(4-Phpy)(2)M(CN)(4)·2G (where 4-Phpy=4-phenylpyridine, M=Cd or Hg and G=1,4-dioxane) have been prepared in powder form and their FT-IR and Raman spectra have been reported. The results suggest that these compounds are similar in structure to the Hofmann-T(d) type clathrates.     

Solanopubamine,a rare steroidal alkaloid from Solanum schimperianum: Synthesis of some new alkyl and acyl derivatives,their anticancer and antimicrobial evaluation

Solanopubamine (3β-amino-5α, 22αH, 25βH-solanidan-23β-ol), a steroidal alkaloid was isolated from the alkaloidal fraction of Solanum schimperianum in significant yield. Its structure was established by IR, positive ESI-MS, 1D and 2D NMR. The presence of -3β-NH₂ and -23β-OH groups was achieved through methylation, acetylation or coupling with octadecanoic and undec-11-enoic acids to produce six derivatives (2–7). Their structures were confirmed by spectroscopic analyses. Solanopubamine and semi-synthetic analogs are investigated for their in vitro cytotoxicity against a panel of human cancer cell lines and anti-microbial activity. Solanopubamine showed good antifungal activity only against Candida albicans and C. tenuis with MIC of 12.5 μg/mL. Semi-synthesized compounds (2–7) have failed to show anti-tumor and anti-microbial activities.     

Inorganic arsenic speciation in various water samples with GFAAS using coprecipitation

A simple, economic and sensitive method for selective determination of As(III) and As(V) in water samples is described. The method is based on selective coprecipitation of As(III) with Ce(IV) hydroxide in presence of an ammonia/ammonium buffer at pH 9. The coprecipitant was collected on a 0.45 µm membrane filter, dissolved with 0.5 mL of conc. nitric acid and the solution was completed to 2 or 5 mL with distilled water. As(III) in the final solutions was determined by graphite furnace atomic absorption spectrometry (GFAAS). Under the working condition, As(V) was not coprecipitated. Total inorganic arsenic was determined after the reduction of As(V) to As(III) with NaI. The concentration of As(V) was calculated by the difference of the concentrations obtained by the above determinations. Both the determination of arsenic with GF-AAS in presence of cerium and the coprecipitation of arsenic with Ce(IV) hydroxide were optimised. The suitability of the method for determining inorganic arsenic species was checked by analysis of water samples spiked with 4–20 µg L^?1 each of As(III) and As(V). The preconcentration factor was found to be 75 with quantitative recovery (≥95%). The accuracy of the present method was controlled with a reference method based on TXRF. The relative error was under 5%. The relative standard deviations for the replicate analysis ( n?=?5) ranged from 4.3 to 8.0% for both As(III) and As(V) in the water samples. The limit of detection (3σ) for both As (III) and As(V) were 0.05 µg L^?1. The proposed method produced satisfactory results for the analysis of inorganic arsenic species in drinking water, wastewater and hot spring water samples.     

Cyclohexenones Through Regioselective Addition of 1,3-Dicarbonyl Compounds to Terpenoid-Like Bischalcones

Terpenoid-like bischalcones (3 and 4) were synthesized from the reaction of α- and β-ionones and benzaldehydes in excellent yields. The Michael addition of 1,3-dicarbonyl compounds to bischalcones (3 and 4) resulted in the formation of cyclohexenones derivatives (10a–d and 14a, b) via regioselective addition of 1,3-dicarbonyls and then cyclization.     

Synthesis of novel iodo derived bicalutamide analogs

A series of optically active nonsteroidal selective androgen receptor modulators with structures analogous to bicalutamide was prepared by replacing the trifluoromethyl group with iodine and the sulfonyl linker by oxygen.     

Stressed Kinetics of Nanoemulsion Formulation Encapsulated Ropinirole with a Validated Ultra High Performance Liquid Chromatography–Synapt Mass Spectrometry (UPLC‐MS/MS ESI‐Q‐TOF)

A highly sensitive ultra high pressure liquid chromatography (UHPLC‐MSMS) method for estimation of ropinirole in rat brain homogenate and plasma has been validated. The method was successfully used for the degradation kinetics in different stress condition and regulated temperature. The chromatographic separation was achieved using isocratic mobile phase, consisting of acetonitrile–2mM ammoniumacetate (28:72 v/v; 0.25 mL min^?1). The mass spectrometer was operated in synapt mass spectrometry mode via positive electrospray ionization using the transitions m/z 260 → m/z 261 for ropinirole, and m/z 324.39 → m/z 262.161 as a parent ion of escitalopram (IS). The assay for ropinirole was linear over the range of 0.5–100 ng mL^?1 (r²; 0.999). The intra‐ and inter day precisions were less than 11.2% in terms of relative standard deviation (R.S.D.), and the accuracy was within ±6.4% in terms of relative error (RE). The mean extraction‐efficiency of QC samples (MQC, 8 ng/mL) was ≥80%. The lower limit of quantification (LLOQ) was 0.049 ng/mL where as lower limit of detection (LLOD) was 0.016 ng/mL. All the peaks of degradation were well resolved. The degradation kinetics of ropinirole, showed highest stability (t_1/2 256.66/h; t_0.9, 39.11/h) in acidic medium, lower stability in alkaline environment (t_1/2, 103.43/h; t_0.9, 15.76/h) and highly susceptible in oxidative environment (t_1/2, 21.58/h; t_0.9, 3.28/h). The applicability of this assay was demonstrated and successfully applied for pharmacokinetic profiling of ropinirole in Wister rat brain homogenate after intranasal administration.