Regiospecific synthesis of novel spiro-pyrimidobarbiturates with promising antibacterial activities

In this work, a novel series of 9-amino-7-aryl-11-imino-2,4,8,10-tetraazaspiro[5.5]undeca-7,9-diene-1,3,5-triones 3a-l was synthesized via the treatment of cyanoguanidine 1 with respective arylidene barbituric acids 2a-l in dry pyridine. The products were evaluated for in vitro antibacterial activity against Bacillus cereus (+G), Staphylococcus aureus (+G), Pseudomonas aeruginosa (−G) and Escherichia coli (−G). The results showed that some of the tested products are promising antibacterial drugs.     

Novel sulfenamides as promising acetylcholinesterase inhibitors

Several sulfenamide derivatives were designed as possible acetylcholinesterase (AChE) inhibitors. New sulfenamides were synthesized and proved to be stable under the physiological conditions used in the enzymatic assays. N‐benzyl‐2‐benzoxazolylsulfenamide (8) and N‐benzyl‐2‐benzimidazolylsulfenamide (9) revealed anti‐AChE activity with IC₅₀ values of 0.6 and 0.8 μM, respectively, values of the same magnitude as those reported for galantamine and tacrine. The affinity for the biological site was evaluated in terms of interaction/partition toward sodium dodecyl sulfate (SDS) micelles. The inhibitory activity profiles were reasoned in terms of both partition toward a hydrophobic anionic environment and molecular geometry. The X? CSN dihedral angle deviations from collinearity stood out as a major parameter linked to enzyme specificity. J. Heterocyclic Chem., (2011).     

Facile synthesis of Cu-LDH with different Cu/Al molar ratios: application as antibacterial inhibitors

Research on Chemical Intermediates - A range of Cu-LDHs has been synthesized by co-precipitation using metal nitrate precursors and sodium carbonate under varying molar ratios Cu/Al...     

Facile synthesis of 9-substituted 9-deazapurines as potential purine nucleoside phosphorylase inhibitors

A facile synthesis of 9-substituted 9-deazapurines as potential inhibitors of purine nucleoside phosphorylase has been achieved by the direct Friedel-Crafts aroylation or arylmethylation of 9-deazapurines using trifluoromethanesulfonic acid as catalyst. The aroylated 9-deazapurines could be transformed into the corresponding 9-aryimethyl derivatives by the Wolff-Kishner reaction. A novel synthesis of 9-deazahypoxanthine was also developed by treatment of 4-hydroxy-5-phenylazo-6-methylpyrimidin-2-thione with triethyl orthoformate in trifluoroacetic acid (TFA) to yield 8-oxo-7H-2-phenylpyrimido[5,4-c]pyridazin-6-thione followed by Raney nickel reduction.     

Facile hydrothermal-thermal conversion synthesis of CaSiO3 nanowires as promising structure and function integrated photoluminescent host candidate

A facile green hydrothermal-thermal conversion method was developed for the uniform high aspect ratio CaSiO₃ nanowires as promising structure and function integrated photoluminescent host, without any organic additive.     

Facile and regioselective synthesis of novel 2,4-disubstituted-5-fluoropyrimidines as potential kinase inhibitors

2,4-Disubstituted-5-fluoropyrimidine is a biologically active molecular core seen in various anticancer agents such as 5-fluorouracil (5-FU). As part of a programme aimed at discovering kinase inhibitors, routes to two series of novel compounds (5-fluoropyrimidine-2-carboxamides and 5-fluoropyrimidine-4-carboxamides) were successfully executed. For the first series, regioselective substitution at the 4-position of the pyrimidine with an amine (HNR¹R²) was achieved, followed by preparation of the amide at the 2-position. The route to the second series involved introduction of the methoxy protecting group at the 4-position, which allowed subsequent amine substitution to occur at the 2-position. The 4-amide substituent was finally introduced by direct conversion of the 4-methoxy into a 4-chloro group followed by transformation into an amide by palladium catalysis.     

Facile synthesis of novel heterocyclic compounds based on pyridine moiety with pharmaceutical activities

A novel run of fused heterocyclic derivatives containing pyridine moieties has been disclosed by allowing 2-amino-4-phenyl-6-(phenyl amino)pyridine-3,5-dicarbonitrile 1 to undergo annulation reactions with different reagents. Most of synthesized compounds have moderate to strong antitumor activity against HePG-2 and MCF-7. Moreover, MOE 2014.09 software was used to run the computational studies to support the biological activity results. The assigned structures for all the newly prepared derivatives were ascertained on the basis of elemental analyses and spectral data.     

Molecular design,synthesis and biological activities of amidines as new ketol-acid reductoisomerase inhibitors

Diamidine （A） was identified in our in vitro bio-assay as a possible inhibitor of ketol-acid reductoisomerase （KARI） from the ACD database search based on the known three-dimensional crystal structure of KARI. An investigation on interaction of A on KARI active sites, led to the design and synthesis of 15 novel monoamidines. Some of those showed better biological activity than A on rice KARI （in vitro） and in greenhouse herbicidal tests （in vivo）. The structure-biological activity relationship was investigated, which provides valuable information to further study of potential KARI inhibitors.     

Design, synthesis and biological evaluation of potent azadipeptide nitrile inhibitors and activity-based probes as promising anti-Trypanosoma brucei agents

Trypanosoma cruzi and Trypanosoma brucei are parasites that cause Chagas disease and African sleeping sickness, respectively. There is an urgent need for the development of new drugs against both diseases due to the lack of adequate cures and emerging drug resistance. One promising strategy for the discovery of small-molecule therapeutics against parasitic diseases has been to target the major cysteine proteases such as cruzain for T. cruzi, and rhodesain/TbCatB for T. brucei. Azadipeptide nitriles belong to a novel class of extremely potent cysteine protease inhibitors against papain-like proteases. We herein report the design, synthesis, and evaluation of a series of azanitrile-containing compounds, most of which were shown to potently inhibit both recombinant cruzain and rhodesain at low nanomolar/picomolar ranges. A strong correlation between the potency of rhodesain inhibition (i.e., target-based screening) and trypanocidal activity (i.e., whole-organism-based screening) of the compounds was observed. To facilitate detailed studies of this important class of inhibitors, selected hit compounds from our screenings were chemically converted into activity-based probes (ABPs), which were subsequently used for in situ proteome profiling and cellular localization studies to further elucidate potential cellular targets (on and off) in both the disease-relevant bloodstream form (BSF) and the insect-residing procyclic form (PCF) of Trypanosoma brucei. Overall, the inhibitors presented herein show great promise as a new class of anti-trypanosome agents, which possess better activities than existing drugs. The activity-based probes generated from this study could also serve as valuable tools for parasite-based proteome profiling studies, as well as bioimaging agents for studies of cellular uptake and distribution of these drug candidates. Our studies therefore provide a good starting point for further development of these azanitrile-containing compounds as potential anti-parasitic agents.     

Convenient synthesis of novel sulfonamide derivatives as promising anticancer agents

Novel sulfonamide derivatives have been synthesized from the readily accessible N-(4-acetylphenyl)benzenesulfonamide (1) . Condensation of 1 with phenylhydrazine in refluxing ethyl alcohol gave the corresponding phenylhydrazone 2 , which was then added to the Vilsmeier-Haack reagent (POCl₃/DMF) to give the 4-formylpyrazole derivative 3 . Fusion of 1 with thiourea in the presence of iodine at 130°C afforded the 2-aminothiazole derivative 4 . Refluxing 1 with an excess of N, N-dimethylformamide dimethyl acetal furnished the enaminone 5 . The chemical reactivity of enaminone 5 toward some nitrogen and carbon nucleophiles has been studied to obtain polyfunctionalized heteroaromatic systems bearing a sulfonamide moiety. Besides, the enaminone 5 undergoes the Gewald reaction and reacts with ethyl cyanoacetate and elemental sulfur in the presence of morpholine to yield the 2-aminothiophene derivative 18 . Moreover, the utility of 5 for the synthesis of 4-(phenylsulfonamido)benzoic acid (19) was investigated. The synthesized sulfonamides were evaluated for their in vitro cytotoxic activities against two human cell lines, MCF-7 (breast adenocarcinoma cells) and RPE-1 (normal retina pigmented epithelium cells). The results revealed that compounds 1-3 , 6-8 , 10 , 12b , 18 , 19 , and 21 have a potent cytotoxic effect on MCF-7 and less on RPE-1 cells compared to the positive control doxorubicin®.     

Structure-activity relationships of estrogen derivatives as aromatase inhibitors. Effects of heterocyclic substituents

Aromatase, which is responsible for the conversion of androgens to estrogens, is a potential therapeutic target for the selective lowering estrogen level in patients with estrogen-dependent breast cancer. We prepared and tested series of the pyridine- and other heterocyclic ring-containing derivatives of 2- and 4-aminoestrones, estrone, and estradiol, compounds 5, 10, 12 and 15. The isonicotinyl derivatives of 2- and 4-aminoestrone, compounds 5c and 10c, were fairly potent competitive inhibitors of aromatase (K(i), 2.1+/-0.14 and 1.53+/-0.08 microM for 5c and 10c, respectively) and other compounds did not show, to a significant extent, the aromatase inhibitory activity. This result suggests that the isonicotinyl-substituted derivatives 5c and 10c would be accessible to the active site of aromatase.     

Acrosin structure-based design,synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

A series of 7-azaindol derivatives were designed based on the homologous 3D model of human acrosin.These compounds were synthesized and evaluated for their human acrosin inhibitory activities in vitro.Compounds 7a,7i,7j,7k and 7n showed highly inhibitory activity against human acrosin.The three-dimensional structure-activity relationship was investigated through a CoMFA model,which provided valuable information to further study of potential human acrosin inhibitors.     

Facile synthesis of heterocycles via 2-picolinium bromide and antimicrobial activities of the products

The 2-picolinium N-ylide 4, generated in situ from the N-acylmethyl-2-picolinium bromide 3, underwent cycloaddition to N-phenylmaleimide or carbon disulfide to give the corresponding cycloadducts 6 and 8, respectively similar reactions of compound 3 with some electron-deficient alkenes in the presence of MnO(2) yielded the products 11 and 12. In addition, reaction of 4 with arylidene cyanothioacetamide andmalononitrile derivatives afforded the thiophene and aniline derivatives 15 and 17, respectively. Heating of picolinium bromide 3 with triethylamine in benzene furnished 2-(2-thienyl)indolizine (18). The structures of the isolated products were confirmed by elemental analysis as well as by (1)H- and (13)C-NMR, IR, and MS data. Both the stereochemistry and the regioselectivity of the studied reactions are discussed. The biological activity of the newly synthesized compounds was examined and showed promising results.     

十五碳内酯的简易合成法

以中国西南地区的油料植物蒜头果油(Kernal oil),经皂化得到的二十四碳-15-烯酸为原料.通过臭氧化和硼氢化还原反应得到ω-羟基十五碳烷酸.以碳酸钾为催化剂,聚乙二醇为相转移催化剂使后者缩聚和解聚可以91%的得率制得十五碳内酯.在合成过程中,用正交试验和方差分析找出最佳实验条件.该大环内酯具有良好的定香作用.     

Facile synthesis of troilite

Low-temperature synthetic pathways can result in crystallization of metastable materials. These methods have been widely explored for the preparation of metal oxides. Adaptation of nonhydrolytic sol-gel chemistry to non-oxide systems offers an elegant route to transition-metal sulfides. The method can be exploited for the facile and reproducible synthesis of iron sulfide crystallizing in the troilite structure. This phase is only found in meteorites and planets and has previously been obtained by high-temperature or high-energy ball-milling methods. "Nonhydrolytic" sol-gel processing results in direct crystallization of troilite with no need for further calcination.     

Facile synthesis of gamma-alkylidenebutenolides

In this paper, a novel route to gamma-alkylidenebutenolides (gamma-AIBs) by way of stereoselective vinylogous aldol reaction of the unactivated butenolide in simple and general conditions is reported.     

Facile synthesis of furobenzothiazepines

The reaction of methyl 5-(2-isocyanatophenylthio)-2-furancarboxylate 2 with N-methylpiperazine gave 5-(2-N-piperazinocarbamoylphenylthio)-2-furancarboxylate 3a . Furthermore, 4-N-methylpiperazinyl-2-methoxycarbonylfuro[2,3-b][1,5]benzothiazepine 4a was obtained by the Bischler-Napieralski reaction of 3a with phosphorus oxychloride in the present of phosphorus pentoxide. Three furobenzothiazepines could be obtained using the same method. Based on the pharmacological studies of these compounds, it was found that 4-morpholinyl-2-methoxycarbonylfuro[2,3-b][1,5]benzothiazepine 4b had anti-inflammatory activity similar to flufenamic acid.     

Facile microwave route for the synthesis of CuS/CQDs/g-C3N4NS as a novel promising cathodic electrochemiluminescence detection of imidacloprid

Journal of Solid State Electrochemistry - In this study, a novel electrochemical luminescence based on ternary nanocomposite as CuS/CQDs/g-C3N4NS was demonstrated for accurate determination of...     

Ethyl acrylate copolymers as promising porogens for the synthesis of polydimethacrylates with controlled porous structures

The crosslinking radical polymerization of triethylene glycol dimethacrylate in bulk in the presence of 0–40 wt % ethyl acrylate-based copolymers of various compositions is studied, and some structuralphysical properties of the crosslinked polymers are investigated. The quantitative characteristics of their porous structures, such as the specific surface areas and the total pore volumes, are measured via the low-temperature adsorption of nitrogen. During sol-gel analysis, polymer additives are removed from network polymers with the use of benzene and pores with sizes from 4 to 500 nm occupy their places. The maximum specific surface area is approximately 17 m²/g. It is found that the specific surface area and total pore volume depend on the content of the polymer additive in the initial composition.