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Molecules, Volume 14, Issue 7 (July 2009) – 28 articles , Pages 2306-2683

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266 KiB  
Article
Mechanism of Introduction of Exogenous Genes into Cultured Cells Using DEAE-Dextran-MMA Graft Copolymer as Non-Viral Gene Carrier
by Yuki Eshita, Junko Higashihara, Masayasu Onishi, Masaaki Mizuno, Jun Yoshida, Tomohiko Takasaki, Naoji Kubota and Yasuhiko Onishi
Molecules 2009, 14(7), 2669-2683; https://doi.org/10.3390/molecules14072669 - 23 Jul 2009
Cited by 18 | Viewed by 17617
Abstract
Comparative investigations were carried out regarding the efficiency of introduction of exogenous genes into cultured cells using a cationic polysaccharide DEAE-dextran-MMA (methyl methacrylate ester) graft copolymer (2-diethylaminoethyl-dextran-methyl methacrylate graft copolymer; DDMC) as a nonviral carrier for gene introduction. The results confirmed that the [...] Read more.
Comparative investigations were carried out regarding the efficiency of introduction of exogenous genes into cultured cells using a cationic polysaccharide DEAE-dextran-MMA (methyl methacrylate ester) graft copolymer (2-diethylaminoethyl-dextran-methyl methacrylate graft copolymer; DDMC) as a nonviral carrier for gene introduction. The results confirmed that the gene introduction efficiency was improved with DDMC relative to DEAE-dextran. Comparative investigations were carried out using various concentrations of DDMC and DNA in the introduction of DNA encoding luciferase (pGL3 control vector; Promega) into COS-7 cells derived from African green monkey kidney cells. The complex formation reaction is thought to be directly proportional to the transformation rate, but the complex formation reaction between DDMC and DNA is significantly influenced by hydrophobic bonding strength along with hydrogen bonding strength and Coulomb forces due to the hydrophobicity of the grafted MMA sections. It is thought that the reaction is a Michaelis-Menten type complex formation reaction described by the following equation: Complex amount = K1 (DNA concentration)(DDMC concentration). In support of this equation, it was confirmed that the amount of formed complex was proportional to the RLU value. Full article
(This article belongs to the Special Issue Macromolecules: Chemistry, Medicinal and Functional Materials)
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<p>Transfection of COS-7 cells with sample 1 of DEAE-dextran and DEAE-dextran-MMA graft copolymer. The grafting rate is 130% for sample 2 at 10 mg/mL, sample 3 at 20 mg/mL, and sample 4 at 28.6 mg/mL.</p> Full article ">Figure 2
<p>DNase degradation times for foreign DNA complex with DEAE-dextran-MMA graft copolymer and DEAE-dextran, respectively. DNase I degrades both double-stranded and single-stranded DNA endonucleolytically, producing 3´-OH oligonucleotides. Toluidine Blue (TB) is isolated in water from DNA after the degradation, as the DNA is stained with TB. This shows the absorbance of TB isolated from DNA in each sample in the water with a spectrophotometer.</p> Full article ">Figure 3
<p>Transfection of COS-7 cells with samples of DEAE-dextran and DEAE-dextran-MMA graft copolymer having a grafting rate of 130% and including 0.075 μg of DNA. Maximum luciferase expression within each experiment was set at 100%.</p> Full article ">Figure 4
<p>Infra-Red absorption spectra: a, complex of DDMC/DNA; b, DDMC; c, complex of DEAE-dextran/DNA; d, DEAE-dextran.</p> Full article ">Figure 5
<p>Schematic drawing of putative delivery pathways for foreign DNA complex with DEAE-dextran-MMA graft copolymer.</p> Full article ">
323 KiB  
Article
Electronic Structure of the Azide Group in 3¢-Azido-3¢-deoxythymidine (AZT) Compared to Small Azide Compounds
by Fang-Fang Chen and Feng Wang
Molecules 2009, 14(7), 2656-2668; https://doi.org/10.3390/molecules14072656 - 22 Jul 2009
Cited by 37 | Viewed by 19007
Abstract
Theoretical calculations for some structural and electronic properties of the azide moiety in the nucleoside reverse transcriptase (RT) inhibitor 3¢-azido-3¢-deoxythymidine (AZT) are reported. These properties, which include geometrical properties in three dimensional space, Hirshfeld charges, electrostatic potential (MEP), vibrational frequencies, and core and [...] Read more.
Theoretical calculations for some structural and electronic properties of the azide moiety in the nucleoside reverse transcriptase (RT) inhibitor 3¢-azido-3¢-deoxythymidine (AZT) are reported. These properties, which include geometrical properties in three dimensional space, Hirshfeld charges, electrostatic potential (MEP), vibrational frequencies, and core and valence ionization spectra, are employed to study how the azide group is affected by the presence of a larger fragment. For this purpose, two small but important organic azides, hydrazoic acid and methyl azide, are also considered. The general features of trans Cs configuration for RNNN fragments[1] is distorted in the large AZT bio-molecule. Hirshfeld charge analysis shows charges are reallocated more evenly on azide when the donor group R is not a single atom. Infrared and photoelectron spectra reveal different aspects of the compounds. In conclusion, the electronic structural properties of the compounds depend on the specific property, the local structure and chemical environment of a species. Full article
(This article belongs to the Special Issue Macromolecules: Chemistry, Medicinal and Functional Materials)
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<p>Structures and Hirshfeld charges of: (a) hydrazoic acid (HN3), (b) methyl azide (CH3N3) and (c) 3′-Azido-3′-deoxythymidine (AZT).</p> Full article ">Figure 2
<p>Molecular electrostatic potentials (MEPs) of (a) HN<sub>3</sub>, (b) CH<sub>3</sub>N<sub>3</sub>, and (c) AZT.</p> Full article ">Figure 3
<p>The simulated N-K binding energy spectra of AZT, CH<sub>3</sub>N<sub>3</sub> and HN<sub>3</sub>.</p> Full article ">Figure 4
<p>Simulated valence binding energy spectra (FWHM=0.40 eV) of AZT, CH<sub>3</sub>N<sub>3</sub> and HN<sub>3</sub>, based on SAOP/et-pVQZ calculations. The azide dominant orbitals are labeled in the spectra with selected orbitals contour plots.</p> Full article ">
144 KiB  
Article
A New Friedelane Type Triterpene from Euonymus hederaceus
by Cui-Rong Sun, He-Jiao Hu, Run-Sheng Xu, Jie-Hong Yang and Hai-Tong Wan
Molecules 2009, 14(7), 2650-2655; https://doi.org/10.3390/molecules14072650 - 17 Jul 2009
Cited by 17 | Viewed by 11499
Abstract
Euonymus hederaceus is distributed widely in the south of China; its stems and leaves have been used as folk medicines to treat many diseases such as renal deficiency and chronic diarrhea, traumatic injury, and abnormal menstruation. Chemical investigation of the leaves and stems [...] Read more.
Euonymus hederaceus is distributed widely in the south of China; its stems and leaves have been used as folk medicines to treat many diseases such as renal deficiency and chronic diarrhea, traumatic injury, and abnormal menstruation. Chemical investigation of the leaves and stems of Euonymus hederaceus resulted in the isolation forthe first time and characterization of a new friedelane type triterpene with a molecular mass of 472 and molecular formula of C30H48O4 by high resolution mass spectrometry. The 1H-NMR 13C-NMR and DEPT1350 spectra matched the characteristic data of the proposed triterpene skeleton.The compound was finally identified as 28-hydroxyfriedelan-3-one-29-oic acid on the basis of spectroscopic evidence, including two dimensional nuclear magnetic resonance as well as its IR spectrum. Full article
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<p>The structure of 28-hydroxy-friedelan-3-one.</p> Full article ">Figure 2
<p>The structure of compound <b>1</b>.</p> Full article ">Figure 3
<p>The chair-chair conformation of compound <b>1</b>.</p> Full article ">
638 KiB  
Article
Experimental and Computational Studies on Non-Covalent Imprinted Microspheres as Recognition System for Nicotinamide Molecules
by Roberta Del Sole, Maria Rosaria Lazzoi, Mario Arnone, Fabio Della Sala, Donato Cannoletta and Giuseppe Vasapollo
Molecules 2009, 14(7), 2632-2649; https://doi.org/10.3390/molecules14072632 - 17 Jul 2009
Cited by 41 | Viewed by 16131
Abstract
Molecularly imprinted microspheres obtained by precipitation polymerization using nicotinamide (nia) as template have been prepared and characterised by SEM. How various experimental parameters can affect microsphere morphology, reaction yield and re-binding capacity have been evaluated. Pre-polymerization interactions between template and functional monomer in [...] Read more.
Molecularly imprinted microspheres obtained by precipitation polymerization using nicotinamide (nia) as template have been prepared and characterised by SEM. How various experimental parameters can affect microsphere morphology, reaction yield and re-binding capacity have been evaluated. Pre-polymerization interactions between template and functional monomer in chloroform and MeCN have been studied by 1H-NMR. The results suggest that the interaction between nia and methacrylic acid (MAA) is mainly based on hydrogen-bonding between amide protons and MAA. Computational density functional theory (DFT) studies on MAA-nia complexes have been also performed to better understand hydrogen-bonding interactions. The imprinted activity of the microspheres, synthesized in chloroform or acetonitrile (MeCN), has been evaluated by spectrophotometric analysis of nia solutions when chloroform or MeCN are used as incubation solvents. The results suggest that MeCN interferes with hydrogen bonding between template and MAA during either the polymerization step or re-binding process as also observed from theoretical results. Finally, the selectivity towards selected nia analogues has been also confirmed. Full article
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<p>Scanning electron microscopy (SEM) images of P1, P3, P6 and P7 polymers (20,000X).</p> Full article ">Figure 2
<p>Schematic representation of all possible 1:1 complexes between nia template and MAA functional monomer.</p> Full article ">Figure 3
<p>The most stable prepolymerization-complex structures for a ratio of 1:2, 1:3 and 1:4 between nia template and MAA functional monomer.</p> Full article ">Figure 4
<p>The hydrogen bond between MeCN and nia.</p> Full article ">Figure 5
<p>Binding capacity in CHCl<sub>3</sub> of imprinted polymer P1 and non-imprinted polymer N-P1 versus nia concentration.</p> Full article ">Figure 6
<p>Binding capacity of imprinted polymer P1 in CHCl<sub>3</sub> and MeCN versus nia concentration.</p> Full article ">Figure 7
<p>Binding capacity of imprinted polymer P1 versus different nitrogen bases.</p> Full article ">Figure 8
<p>The possible binding sites for the functional monomer MAA to the nicotinamide template molecule.</p> Full article ">
138 KiB  
Article
Synthesis and Biological Activity of Some New 1,3,4-Thiadiazole and 1,2,4-Triazole Compounds Containing a Phenylalanine Moiety
by Mihaela Moise, Valeriu Sunel, Lenuta Profire, Marcel Popa, Jacques Desbrieres and Cristian Peptu
Molecules 2009, 14(7), 2621-2631; https://doi.org/10.3390/molecules14072621 - 16 Jul 2009
Cited by 69 | Viewed by 18223
Abstract
New 1,3,4-thiadiazole, 6, 7 and 1,2,4-triazole derivatives, 8, 9 containing a phenylalanine moiety have been synthesized by intramolecular cyclization of 1,4-disubstituted thiosemicarbazides, 4, 5, in acid and alkaline media, respectively; the thiosemicarbazides were obtained by reaction of hydrazide 3 with appropriate aromatic isothiocyanates. [...] Read more.
New 1,3,4-thiadiazole, 6, 7 and 1,2,4-triazole derivatives, 8, 9 containing a phenylalanine moiety have been synthesized by intramolecular cyclization of 1,4-disubstituted thiosemicarbazides, 4, 5, in acid and alkaline media, respectively; the thiosemicarbazides were obtained by reaction of hydrazide 3 with appropriate aromatic isothiocyanates. The toxicity of the synthesized compounds was evaluated and the anti-inflammatory study of the triazole compound 9 established an appreciable anti-inflammatory activity that is comparable with that of other nonsteroidal anti-inflammatory agents. Full article
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<p>Synthesis of oxazolone <b>2.</b></p> Full article ">Figure 2
<p>Synthesis of hydrazide <b>3.</b></p> Full article ">Figure 3
<p>Synthesis of thiosemicarbazides <b>4, 5.</b></p> Full article ">Figure 4
<p>Synthesis of 1,3,4-thiadiazole (<b>6, 7</b>) and 1,2,4-triazole (<b>8, 9</b>) compounds.</p> Full article ">
324 KiB  
Review
Polymeric Plant-derived Excipients in Drug Delivery
by Carien E. Beneke, Alvaro M. Viljoen and Josias H. Hamman
Molecules 2009, 14(7), 2602-2620; https://doi.org/10.3390/molecules14072602 - 16 Jul 2009
Cited by 273 | Viewed by 26467
Abstract
Drug dosage forms contain many components in addition to the active pharmaceutical ingredient(s) to assist in the manufacturing process as well as to optimise drug delivery. Due to advances in drug delivery technology, excipients are currently included in novel dosage forms to fulfil [...] Read more.
Drug dosage forms contain many components in addition to the active pharmaceutical ingredient(s) to assist in the manufacturing process as well as to optimise drug delivery. Due to advances in drug delivery technology, excipients are currently included in novel dosage forms to fulfil specific functions and in some cases they directly or indirectly influence the extent and/or rate of drug release and absorption. Since plant polysaccharides comply with many requirements expected of pharmaceutical excipients such as non-toxicity, stability, availability and renewability they are extensively investigated for use in the development of solid oral dosage forms. Furthermore, polysaccharides with varying physicochemical properties can be extracted from plants at relatively low cost and can be chemically modified to suit specific needs. As an example, many polysaccharide-rich plant materials are successfully used as matrix formers in modified release dosage forms. Some natural polysaccharides have even shown environmental-responsive gelation characteristics with the potential to control drug release according to specific therapeutic needs. This review discusses some of the most important plant-derived polymeric compounds that are used or investigated as excipients in drug delivery systems. Full article
(This article belongs to the Special Issue Macromolecules Applied to Pharmaceutics)
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<p>Chemical structure of a) powdered cellulose (n ≈ 500) or microcrystalline cellulose (n ≈ 220) and b) hydroxypropylmethylcellulose.</p> Full article ">Figure 2
<p>Chemical structure of pectin.</p> Full article ">Figure 3
<p>Chemical structure of inulin.</p> Full article ">Figure 4
<p>Chemical structure of alginates.</p> Full article ">Figure 5
<p>Chemical structure of a) λ-carrageenan, b) ι-carrageenan and c) κ-carrageenan.</p> Full article ">Figure 6
<p>Chemical structure of rosin.</p> Full article ">Figure 7
<p>Chemical structure of guar gum.</p> Full article ">Figure 8
<p>Chemical structure of locust bean gum.</p> Full article ">Figure 9
<p>Chemical structure of starch, with a) amylose and b) amylopectin.</p> Full article ">
156 KiB  
Article
Calixpyrrole Derivatives: “Multi Hydrogen Bond” Catalysts for γ-Butenolide Synthesis
by Grazia Cafeo, Margherita De Rosa, Franz H. Kohnke, Annunziata Soriente, Carmen Talotta and Luca Valenti
Molecules 2009, 14(7), 2594-2601; https://doi.org/10.3390/molecules14072594 - 15 Jul 2009
Cited by 25 | Viewed by 14163
Abstract
Calix[4]pyrrole (1), calix[2]m-benzo[4]pyrrole (2), 10α,20β- and 10α,20α- bis(4-nitrophenyl)-calix[4]pyrroles 3 and 4, respectively, were found to exhibit various organocatalytic activities in the diastereoselective vinylogous addition reaction of 2-trimethylsilyloxyfuran (TMSOF, 7) to aldehydes. The γ-hydroxybutenolide products are obtained in fairly good yields and [...] Read more.
Calix[4]pyrrole (1), calix[2]m-benzo[4]pyrrole (2), 10α,20β- and 10α,20α- bis(4-nitrophenyl)-calix[4]pyrroles 3 and 4, respectively, were found to exhibit various organocatalytic activities in the diastereoselective vinylogous addition reaction of 2-trimethylsilyloxyfuran (TMSOF, 7) to aldehydes. The γ-hydroxybutenolide products are obtained in fairly good yields and with moderate diastereoselectivity. The structures of the catalysts, as well as the reaction conditions, strongly influence the efficiency of the reaction. Full article
(This article belongs to the Special Issue Organocatalysis)
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Graphical abstract
Full article ">Figure 1
<p>Diastereoselective addition reaction of TMSOF to aldehydes.</p> Full article ">
340 KiB  
Article
Synthesis, Crystal Structure, and Kinetics of the Thermal Decomposition of the Nickel(II) Complex of the Schiff Base 2-[(4 Methylphenylimino)methyl]-6-methoxyphenol
by Yan-Fang Wang, Jian-Feng Liu, Hui-Duo Xian and Guo-Liang Zhao
Molecules 2009, 14(7), 2582-2593; https://doi.org/10.3390/molecules14072582 - 15 Jul 2009
Cited by 22 | Viewed by 12717
Abstract
A new dinuclear complex, [Ni2(H2O)L4]·5H2O, consisting of chelating bidentate and bridging tridentate coordinated 2-[(4-methylphenylimino)methyl]-6-methoxyphenol (HL) Schiff base ligands and water molecules has been synthesized using a traditional method. The structure of this complex was characterized [...] Read more.
A new dinuclear complex, [Ni2(H2O)L4]·5H2O, consisting of chelating bidentate and bridging tridentate coordinated 2-[(4-methylphenylimino)methyl]-6-methoxyphenol (HL) Schiff base ligands and water molecules has been synthesized using a traditional method. The structure of this complex was characterized by FTIR and UV/Vis spectroscopy and thermogravimetric analyses (TG-DTG) and further confirmed by single-crystal X-ray diffraction. Its crystal structure is of monoclinic system, space group P21/c with a = 13.2837(5) Å, b = 27.3886(10) Å, c = 17.5415(6) Å, α = 90 º, β = 108.429(2) º, γ = 90 º, V = 6054.7(4) Å3, Z = 4. The crystal structure reveals that there is a Ni·Ni core, with a separation of 3.183 Å. Its thermal decomposition kinetics were also studied. Full article
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Graphical abstract
Full article ">Figure 1
<p>The UV/vis spectra of the complex <b>1 </b>and the ligand <b>HL</b>.</p> Full article ">Figure 2
<p>Molecular structure of the complex <b>1</b> (probability of ellipsoid is 30%). All the non-coordinated water molecules are omitted for clarity.</p> Full article ">Figure 3
<p>The three coordinate modes of L in complex <b>1.</b></p> Full article ">Figure 4
<p>The TG-DTG curves of complex <b>1.</b></p> Full article ">Figure 5
<p>Structure of Schiff base ligand.</p> Full article ">
116 KiB  
Article
Extraction of Oil from Wheat Germ by Supercritical CO2
by Alessandra Piras, Antonella Rosa, Danilo Falconieri, Silvia Porcedda, Maria. A. Dessì and Bruno Marongiu
Molecules 2009, 14(7), 2573-2581; https://doi.org/10.3390/molecules14072573 - 15 Jul 2009
Cited by 61 | Viewed by 16683
Abstract
This study examined the supercritical fluid extraction of wheat germ oil. The effects of pressure (200-300 bar at 40 °C) and extraction time on the oil quality/quantity were studied. A comparison was also made between the relative qualities of material obtained by SFE [...] Read more.
This study examined the supercritical fluid extraction of wheat germ oil. The effects of pressure (200-300 bar at 40 °C) and extraction time on the oil quality/quantity were studied. A comparison was also made between the relative qualities of material obtained by SFE and by organic solvent extraction. The extracts were analyzed for α-tocopherol and polyunsaturated fatty acid content. The maximum wheat germ oil yield at about 9% was obtained with supercritical carbon dioxide extraction at 300 bar, while fatty acid and α-tocopherol composition of the extracts was not remarkable affected by either pressure or the extraction method. Full article
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Graphical abstract
Full article ">Figure 1
<p>Effect of pressure on the extraction yield of wheat germ oil: ●, 200 bar and 40 °C; ▲, 250 bar and 40 °C; ♦, 300 bar and 40 °C.</p> Full article ">Figure 2
<p>Effect of extraction method on the yield of wheat germ oil.</p> Full article ">Figure 3
<p>α-Tocopherol amount (expressed as μg/mg oil) measured in wheat germ oil samples obtained by SC-CO<sub>2</sub> (200, 250, and 300 bar) and organic solvent extraction (hexane, methanol, and chloroform-methanol).</p> Full article ">Figure 4
<p>Values (expressed as μg/mg oil) of oleic (18:1), linoleic (18:2), and linolenic (18:3 n-3) acids measured by high-performance liquid chromatography (HPLC-DAD) method in wheat germ oil samples obtained by SC-CO<sub>2</sub> (200, 250, and 300 bar) and organic solvent extraction (hexane, methanol, and chloroform-methanol). p&lt; 0.05, <sup>a</sup> = versus methanol, <sup>b</sup>hexane, <sup>c</sup>chloroform-methanol, <sup>d</sup>200 bar, <sup>e</sup>250 bar; (n = 6).</p> Full article ">
580 KiB  
Article
Diaroyl Tellurides: Synthesis, Structure and NBO Analysis of (2-MeOC6H4CO)2Te – Comparison with Its Sulfur and Selenium Isologues. The First Observation of [MgBr][R(C=Te)O] Salts
by Osamu Niyomura, Shoho Nakaiida, Ryo Yamada, Shinzi Kato, Masaru Ishida, Masahiro Ebihara, Fumio Ando and Jugo Koketsu
Molecules 2009, 14(7), 2555-2572; https://doi.org/10.3390/molecules14072555 - 13 Jul 2009
Cited by 4 | Viewed by 13938
Abstract
A series of aromatic diacyl tellurides were prepared in moderate to good yields by the reactions of sodium orpotassium arenecarbotelluroates with acyl chlorides in acetonitrile. X-ray structure analyses and theoretical calculations of 2-methoxybenzoic anhydride and bis(2-methoxybenzoyl) sulfide, selenide and telluride were carried out. [...] Read more.
A series of aromatic diacyl tellurides were prepared in moderate to good yields by the reactions of sodium orpotassium arenecarbotelluroates with acyl chlorides in acetonitrile. X-ray structure analyses and theoretical calculations of 2-methoxybenzoic anhydride and bis(2-methoxybenzoyl) sulfide, selenide and telluride were carried out. The two 2-MeOC6H4CO moieties of bis(2-methoxybenzoyl) telluride are nearly planar and the two methoxy oxygen atoms intramolecularly coordinate to the central tellurium atom from both side of C(11)-Te(11)-C(22) plane. In contrast, the oxygen and sulfur isologues (2-MeOC6H4CO)2E (E = O, S), show that one of the two methoxy oxygen atoms contacts with the oxygen atom of the carbonyl group connected to the same benzene ring. The structure of di(2-methoxybenzoyl) selenide which was obtained by MO calculation resembles that of tellurium isologues rather than the corresponding oxygen and sulfur isologues. The reactions of di(aroyl) tellurides with Grignard reagents lead to the formation of tellurocarboxylato magnesium complexes [MgBr][R(C=Te)O]. Full article
(This article belongs to the Special Issue Selenium and Tellurium Chemistry)
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Figure 1
<p>ORTEP drawings of (a) bis(2-methoxybenzoyl) telluride (<b>4f</b>), (b) 2-methoxy-benzoic anhydride (<b>5</b>) and (c) bis(2-methoxybenzoyl) sulfide (<b>6</b>). The thermal ellipsoid plots represent 50% probability.</p> Full article ">Figure 2
<p>The optimized structure of (2-MeOC<sub>6</sub>H<sub>4</sub>CO)<sub>2</sub>Te (<b>7</b>) calculated at the RHF/LANL-2dz level. Distances are in angstrom (Å) and angles (°). Torsion angles: O4-C2-C3-O5 = 63.5°; C2-Se1-O18-C8 = 24.2° in degrees (for the other distances and angles: see <a href="#molecules-14-02555-t003" class="html-table">Table 3</a>).</p> Full article ">Figure 3
<p>(a) Packing and (b) intermolecular short contacts of (2-MeOC<sub>6</sub>H<sub>4</sub>CO)<sub>2</sub>Te (<b>4f</b>), view down to <span class="html-italic">c</span>-axis. Green, red, yellow and gray balls are tellurium, oxygen, sulfur and carbon atoms, respectively. For (a), hydrogen atoms are omitted for clarity and molecules <b>4f-A</b> and <b>4f-B</b> are enantiomorphic with each other. For (b), red and light blue dotted lines show intermolecular short contacts.</p> Full article ">Figure 4
<p>(a) Packing and (b) intermolecular short contacts of (2-MeOC<sub>6</sub>H<sub>4</sub>CO)<sub>2</sub>O (5) view down to <span class="html-italic">a</span>-axis. Red, gray and white balls are oxygen, carbon and hydrogen atoms, respectively. For (a), hydrogen atoms are omitted for clarity and molecules 5-A, <b>5-A'</b>, <b>5-B</b> and <b>5-B'</b> are enantiomorphic with each other. For (b), red dotted lines show intermolecular short contacts.</p> Full article ">Figure 5
<p>(a) Packings and (b) intermolecular short contacts of (2-MeOC<sub>6</sub>H<sub>4</sub>CO)<sub>2</sub>S (<b>6</b>) view down to <span class="html-italic">a</span>-axis. Yellow, red, gray and white balls are sulfur, oxygen, carbon and hydrogen atoms, respectively. For (a), hydrogen atoms are omitted for clarity and molecules <b>6-A</b> and <b>6-B</b> are enantiomorphic with each other. For (b), red dotted lines show intermolecular short contacts.</p> Full article ">Figure 6
<p>Synthesis of diacyl tellurides <b>4a-k</b>.</p> Full article ">Figure 7
<p>Reactions of bis(2-methoxybenzoyl) telluride (<b>4f</b>) with Grignard reagents.</p> Full article ">Figure 8
<p>A possible mechanism for the reactions of (2-MeOC<sub>6</sub>H<sub>4</sub>CO)<sub>2</sub> Te (<b>4f</b>) with Grignard reagents.</p> Full article ">
333 KiB  
Review
Bacterial Extracellular Polysaccharides Involved in Biofilm Formation
by Barbara Vu, Miao Chen, Russell J. Crawford and Elena P. Ivanova
Molecules 2009, 14(7), 2535-2554; https://doi.org/10.3390/molecules14072535 - 13 Jul 2009
Cited by 888 | Viewed by 47933
Abstract
Extracellular polymeric substances (EPS) produced by microorganisms are a complex mixture of biopolymers primarily consisting of polysaccharides, as well as proteins, nucleic acids, lipids and humic substances. EPS make up the intercellular space of microbial aggregates and form the structure and architecture of [...] Read more.
Extracellular polymeric substances (EPS) produced by microorganisms are a complex mixture of biopolymers primarily consisting of polysaccharides, as well as proteins, nucleic acids, lipids and humic substances. EPS make up the intercellular space of microbial aggregates and form the structure and architecture of the biofilm matrix. The key functions of EPS comprise the mediation of the initial attachment of cells to different substrata and protection against environmental stress and dehydration. The aim of this review is to present a summary of the current status of the research into the role of EPS in bacterial attachment followed by biofilm formation. The latter has a profound impact on an array of biomedical, biotechnology and industrial fields including pharmaceutical and surgical applications, food engineering, bioremediation and biohydrometallurgy. The diverse structural variations of EPS produced by bacteria of different taxonomic lineages, together with examples of biotechnological applications, are discussed. Finally, a range of novel techniques that can be used in studies involving biofilm-specific polysaccharides is discussed. Full article
(This article belongs to the Special Issue Macromolecules: Chemistry, Medicinal and Functional Materials)
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<p>The structure of dextran with branching at C3 [<a href="#B74-molecules-14-02535" class="html-bibr">74</a>].</p> Full article ">Figure 2
<p>The structure of kefiran, the polysaccharide found in kefir grains [<a href="#B75-molecules-14-02535" class="html-bibr">75</a>].</p> Full article ">Figure 3
<p>The structure of bacterial cellulose [<a href="#B80-molecules-14-02535" class="html-bibr">80</a>].</p> Full article ">Figure 4
<p>The primary structure of gellan gum [<a href="#B74-molecules-14-02535" class="html-bibr">74</a>].</p> Full article ">Figure 5
<p>Chemical structure of curdlan [<a href="#B83-molecules-14-02535" class="html-bibr">83</a>].</p> Full article ">Figure 6
<p>The primary structure of welan gum [<a href="#B74-molecules-14-02535" class="html-bibr">74</a>].</p> Full article ">Figure 7
<p>The structure of: (a) the major disaccharide sequence, (b) the minor disaccharide sequence of heparin and (c) the polysaccharide produced by <span class="html-italic">E. coli</span> [<a href="#B85-molecules-14-02535" class="html-bibr">85</a>].</p> Full article ">Figure 8
<p>The structure of (a) <span class="html-italic">β</span>-<span class="html-small-caps">d</span>-mannuronic acid, (b) <span class="html-italic">α</span>-<span class="html-small-caps">l</span>-guluronic acid and <b>(c)</b> alginate [<a href="#B67-molecules-14-02535" class="html-bibr">67</a>].</p> Full article ">Figure 9
<p>The structure of xanthan [<a href="#B68-molecules-14-02535" class="html-bibr">68</a>].</p> Full article ">
348 KiB  
Article
Ionic Liquids: Just Molten Salts After All?
by Hon Man Yau, Si Jia Chan, Stephen R. D. George, James M. Hook, Anna K. Croft and Jason B. Harper
Molecules 2009, 14(7), 2521-2534; https://doi.org/10.3390/molecules14072521 - 13 Jul 2009
Cited by 51 | Viewed by 16302
Abstract
While there has been much effort in recent years to characterise ionic liquids in terms of parameters that are well described for molecular solvents, using these to explain reaction outcomes remains problematic. Herein we propose that many reaction outcomes in ionic liquids may [...] Read more.
While there has been much effort in recent years to characterise ionic liquids in terms of parameters that are well described for molecular solvents, using these to explain reaction outcomes remains problematic. Herein we propose that many reaction outcomes in ionic liquids may be explained by considering the electrostatic interactions present in the solution; that is, by recognising that ionic liquids are salts. This is supported by evidence in the literature, along with studies presented here. Full article
(This article belongs to the Collection Ionic Liquids)
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<p>Nucleophilic substitution of the chloride <b>1</b> to give the ether <b>2</b>, carried out in a mixture of alcohol and ionic liquid.</p> Full article ">Figure 2
<p>Menschutkin reaction of the benzyl bromide <b>3</b> with pyridine.</p> Full article ">Figure 3
<p>Acid-catalysed hydrolysis of benzaldehyde dimethyl acetal <b>5</b>.</p> Full article ">Figure 4
<p>Nitrile oxide cycloaddition of benzonitrile oxide <b>7</b> to ethyl <span class="html-italic">trans</span>-cinnamate <b>8</b> to give the isoxazoles <b>9a</b> and <b>9b</b>.</p> Full article ">
243 KiB  
Article
Tyrosinase Inhibitor Activity of Coumarin-Resveratrol Hybrids
by Antonella Fais, Marcella Corda, Benedetta Era, M. Benedetta Fadda, Maria Joao Matos, Elias Quezada q, Lourdes Santana, Carmen Picciau, Gianni Podda and Giovanna Delogu
Molecules 2009, 14(7), 2514-2520; https://doi.org/10.3390/molecules14072514 - 13 Jul 2009
Cited by 66 | Viewed by 16567
Abstract
In the present work we report on the contribution of the coumarin moiety to tyrosinase inhibition. Coumarin-resveratrol hybrids 1-8 have been resynthesized to investigate the structure-activity relationships and the IC50 values of these compounds were measured. The results showed that these compounds [...] Read more.
In the present work we report on the contribution of the coumarin moiety to tyrosinase inhibition. Coumarin-resveratrol hybrids 1-8 have been resynthesized to investigate the structure-activity relationships and the IC50 values of these compounds were measured. The results showed that these compounds exhibited tyrosinase inhibitory activity. Compound 3-(3’,4’,5’-trihydroxyphenyl)-6,8-dihydroxycoumarin (8)is the most potentcompound (0.27 mM), more so than umbelliferone (0.42 mM), used as reference compound. The kinetic studies revealed that compound 8 caused non-competitive tyrosinase inhibition. Full article
(This article belongs to the Special Issue Coumarins and Xanthones)
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<p>Dixon plot for the inhibition of tyrosinase by compound <b>8</b> with respect <span class="html-small-caps">L</span>-DOPA as substrate at concentrations: (□) 0.5 mM;(▲) 0.25 mM; (○) and 0.1 mM.</p> Full article ">Figure 2
<p>General synthetic route to obtain compounds <b>1</b>-<b>8.</b></p> Full article ">
234 KiB  
Article
Design and Synthesis of Some Thiazolidin-4-ones Based on (7-Hydroxy-2-oxo-2H-chromen-4-yl) Acetic Acid
by Milan Cacic, Maja Molnar, Tomislav Balic, Nela Draca and Valentina Rajkovic
Molecules 2009, 14(7), 2501-2513; https://doi.org/10.3390/molecules14072501 - 10 Jul 2009
Cited by 16 | Viewed by 11406
Abstract
(7-Hydroxy-2-oxo-2H-chromen-4-yl)-acetic acid methyl ester(1) upon reaction with ethyl bromoacetate furnishes (7-ethoxycarbonylmethoxy-2-oxo-2H-chromen-4-yl)-acetic acid methylester (2), which on treatment with 100% hydrazine hydrate yields (7-hydrazinocarbonylmethoxy-2-oxo-2H-chromen-4-yl)-acetic acid hydrazide (3). The condensation of compound 3 with different aromatic aldehydes afforded a [...] Read more.
(7-Hydroxy-2-oxo-2H-chromen-4-yl)-acetic acid methyl ester(1) upon reaction with ethyl bromoacetate furnishes (7-ethoxycarbonylmethoxy-2-oxo-2H-chromen-4-yl)-acetic acid methylester (2), which on treatment with 100% hydrazine hydrate yields (7-hydrazinocarbonylmethoxy-2-oxo-2H-chromen-4-yl)-acetic acid hydrazide (3). The condensation of compound 3 with different aromatic aldehydes afforded a series of [7-(arylidenehydrazinocarbonylmethoxy)-2-oxo-2H-chromen-4-yl]-acetic acid arylidene-hydrazide Schiff’s bases 4a-k. Cyclo-condensation of compounds 4a-k with 2-mercapto-acetic acid in N,N-dimethylformamide in the presence of anhydrous ZnCl2 affordsN-(2-aryl-4-oxothiazolidin-3-yl)-2-(4-(2-aryl-4-oxothiazolidin-3-ylcarbamoyl)-methyl)-2-oxo-2H-chromen-7-yloxy)-acetamides 5a-k. Structure elucidation of the products has been accomplished on the basis of elemental analysis, IR, 1H-NMR and 13C-NMR data. Compounds 4a-k and 5a-k will be screened for their antibacterial activity against both Gram-positive and Gram-negative bacteria and the results reported elsewhere in due course. Full article
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<p>Synthetic route for thiazolidinones <b>5a-k.</b></p> Full article ">
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Article
Leishmanicidal Activity of Aliphatic and Aromatic Lactones: Correlation Structure-Activity
by Marcela Castaño, Wilson Cardona, Winston Quiñones, Sara Robledo and Fernando Echeverri
Molecules 2009, 14(7), 2491-2500; https://doi.org/10.3390/molecules14072491 - 10 Jul 2009
Cited by 15 | Viewed by 12708
Abstract
Several aliphatic and aromatic lactones and two dimers were synthesized using the sequence: allylation - esterification - metathesis. These compounds were active in vitro against intracellular amastigotes of Leishmania panamensis. The structure-activity relationship showed the importance of the aliphatic side chain to [...] Read more.
Several aliphatic and aromatic lactones and two dimers were synthesized using the sequence: allylation - esterification - metathesis. These compounds were active in vitro against intracellular amastigotes of Leishmania panamensis. The structure-activity relationship showed the importance of the aliphatic side chain to enhance the biological activity and to obtain lower cytotoxicity. It was also observed that a decrease in the size of the lactone ring increases the selectivity index. Full article
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<p>Retrosynthetic analysis of the lactone targets.</p> Full article ">Figure 2
<p>Others lactones synthesized.</p> Full article ">Figure 3
<p>Synthesis of dimer <b>7</b>.</p> Full article ">Figure 4
<p>Synthesis of dilactone <b>15</b>.</p> Full article ">
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Article
Identification and Quantification of Flavonoids and Phenolic Acids in Burr Parsley (Caucalis platycarpos L.), Using High-Performance Liquid Chromatography with Diode Array Detection and Electrospray Ionization Mass Spectrometry
by Ana Plazonić, Franz Bucar, Željan Maleš, Ana Mornar, Biljana Nigović and Nikola Kujundžić
Molecules 2009, 14(7), 2466-2490; https://doi.org/10.3390/molecules14072466 - 9 Jul 2009
Cited by 219 | Viewed by 20973
Abstract
A sensitive method coupling high-performance liquid chromatography (HPLC) with diode-array detector (DAD) and electrospray ionization mass spectrometry (MS) was optimized for the separation and identification of phenolic acids, flavonoid glycosides and flavonoid aglycones in the extract of burr parsley (Caucalis platycarpos L.). [...] Read more.
A sensitive method coupling high-performance liquid chromatography (HPLC) with diode-array detector (DAD) and electrospray ionization mass spectrometry (MS) was optimized for the separation and identification of phenolic acids, flavonoid glycosides and flavonoid aglycones in the extract of burr parsley (Caucalis platycarpos L.). Fragmentation behavior of flavonoid glycosides and phenolic acids were investigated using ion trap mass spectrometry in negative electrospray ionization. The MS, MSn and UV data together with HPLC retention time (TR) of phenolic acids and flavonoids allowed structural characterization of these compounds. Caffeoylquinic acid (CQA) isomers, p-coumaroyl-quinic acids (p-CoQA), feruloylquinic acids (FQA), dicaffeoylquinic acids (diCQA), luteolin-7-O-rutinoside, apigenin-7-O-rutinoside as well as isolated chrysoeriol-7-O-rutinoside have been identified as constituents of C. platycarpos for the first time. An accurate, precise and sensitive LC-DAD method for quantification of four phenolic acids (3-O-caffeoylquinic, caffeic, p-coumaric, o-coumaric acid), four flavonoid glycosides (luteolin-7-O-glucoside, apigenin-7-O-glucoside, quercetin-3-O-galactoside, quercetin-3-O-rhamnoside), and three flavonoid aglycones (luteolin, apigenin, chrysoeriol) in C. platycarpos extract was validated in terms of linearity, limit of detection, limit of quantification, precision and accuracy. 3-O-caffeoylquinic acid was the predominant phenolic acid and luteolin-7-O-glucoside was the predominant flavonoid glycoside. Full article
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<p>HPLC chromatogram of standard solution mixture (0.008 mg/mL) at 325 nm.</p> Full article ">Figure 2
<p>HPLC-DAD chromatogram of methanolic extract of <span class="html-italic">C. platycarpos</span>, λ=325 nm (a); TIC chromatogram of methanolic extract of <span class="html-italic">C. platycarpos</span> from HPLC-(-) ESI-MS (b). Peak identities are numbered in <a href="#molecules-14-02466-t004" class="html-table">Table 4</a> and <a href="#molecules-14-02466-t005" class="html-table">Table 5</a>.</p> Full article ">Figure 3
<p>Chemical structure of flavonoids present in <span class="html-italic">C. platycarpos</span>.</p> Full article ">Figure 4
<p>Ion nomenclature and major fragments illustrated on luteolin-7-<span class="html-italic">O</span>-rutinoside.</p> Full article ">Figure 5
<p>Fragmentation of apigenin-7-<span class="html-italic">O</span>-rutinoside.</p> Full article ">Figure 6
<p>Fragmentation of luteolin-7-<span class="html-italic">O</span>-rutinoside.</p> Full article ">Figure 7
<p>Structures of chlorogenic acids and associated cinnamic acids.</p> Full article ">Figure 8
<p>Fragmentation of 4,5-<span class="html-italic">O</span>-dicaffeoylquinic acid.</p> Full article ">Figure 9
<p>The structure of isolated chrysoeriol-7-<span class="html-italic">O-α</span>-<span class="html-small-caps">l</span>-rhamnosyl (1→6)-<span class="html-italic">β</span>-<span class="html-small-caps">d</span>-glucoside.</p> Full article ">Figure 10
<p>Total ion chromatogram of isolated chrysoeriol-7-<span class="html-italic">O-α</span>-<span class="html-small-caps">l</span>-rhamnosyl (1→6)-<span class="html-italic">β</span>-<span class="html-small-caps">d</span>-glucoside.</p> Full article ">Figure 11
<p>Fragmentation of chrysoeriol-7-<span class="html-italic">O-α</span>-<span class="html-small-caps">l</span>-rhamnosyl (1→6)-<span class="html-italic">β</span>-<span class="html-small-caps">d</span>-glucoside.</p> Full article ">
176 KiB  
Article
Chemical Composition of the Essential Oils from the Roots of Erigeron acris L. and Erigeron annuus (L.) Pers.
by Jolanta Nazaruk and Danuta Kalemba
Molecules 2009, 14(7), 2458-2465; https://doi.org/10.3390/molecules14072458 - 9 Jul 2009
Cited by 31 | Viewed by 12297
Abstract
The chemical compositions of essential oils from the roots of Erigeron acris and Erigeron annuus were studied. The essential oils were obtained by hydrodistillation in 1.0% and 0.05% yield, respectively, and analyzed by GC, GC-MS. Fifty four and forty seven constituents were identified. [...] Read more.
The chemical compositions of essential oils from the roots of Erigeron acris and Erigeron annuus were studied. The essential oils were obtained by hydrodistillation in 1.0% and 0.05% yield, respectively, and analyzed by GC, GC-MS. Fifty four and forty seven constituents were identified. Predominant constituents of both oils were poly-acetylene esters: (Z,Z)-matricaria ester (49.4% and 45.9%, respectively) and (Z)-lachnophyllum ester (37.2% and 27.5%, respectively), that were accompanied by their stereoisomers as well as appropriate lactones. Polyacetylenic compounds amounted to 92.1% of E. acris oil and 85.8% of E. annuus oil. Both oils contained the same monoterpene hydrocarbons, amounting to 4.2% and 5.8%, respectively, and traces of almost the same monoterpene oxygenated compounds. The dominant sesquiterpenes in E. acris were elemenes and tricyclic sesquiterpene hydrocarbons, while in E. annuus β-sesquiphellandrene and β-bisabolene dominated. After flash chromatography of essential oil from E. acris, fractions contained acetylene esters and acetylene lactones were obtained. The configuration about double bonds for these compounds has been elucidated on the basis of 1H- and 13C-NMR analysis. Full article
267 KiB  
Article
Synthesis of 3-N-Sugar-substituted-2, 4(1H,3H)-quinazolinedionesas Anti-Angiogenesis Agents
by Conghai Huang, Xiangbao Meng, Jingrong Cui and Zhongjun Li
Molecules 2009, 14(7), 2447-2457; https://doi.org/10.3390/molecules14072447 - 8 Jul 2009
Cited by 7 | Viewed by 8509
Abstract
A series of novel 3-N-sugar-substituted quinazolinediones were synthesizedthrough the cyclization of the intermediate 2-aminobenzamides using triphosgene as the condensing reagent. Their anti-angiogenesis activities were investigated. The compound 3-(2'-aminoglucosyl)-2,4-(1H,3H)-quinazolinedione, (5d) showed good anti-angiogenesis activity. Full article
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<p>Structures of PAQ-22 and the desired 3-N-sugar substituted quinazolinedione derivatives.</p> Full article ">Figure 2
<p>Inbibition of angiogenesis by compound <b>5d</b>.</p> Full article ">Figure 3
<p>The synthetic route to <span class="html-italic">N</span>-sugar-substituted quinazolinedione derivatives.</p> Full article ">
191 KiB  
Article
Synthesis and Antibacterial Activities of New Metronidazole and Imidazole Derivatives
by Abdul Jabar Kh. Atia
Molecules 2009, 14(7), 2431-2446; https://doi.org/10.3390/molecules14072431 - 8 Jul 2009
Cited by 73 | Viewed by 21304
Abstract
New imidazole ring derivatives comprising 1,3-oxazoline, Schiff's bases, thiadiazole, oxadiazole and 1,2,4-triazole moieties are reported. 3-Aminobiimidazol-4-one compounds 7a-c were synthesized by the reaction of compounds 6a-c with hydrazine hydrate. Biimidazole esters 9a-c were converted into biimidazole hydrazide esters 10a-c. Compounds 7a-c and 10a-c [...] Read more.
New imidazole ring derivatives comprising 1,3-oxazoline, Schiff's bases, thiadiazole, oxadiazole and 1,2,4-triazole moieties are reported. 3-Aminobiimidazol-4-one compounds 7a-c were synthesized by the reaction of compounds 6a-c with hydrazine hydrate. Biimidazole esters 9a-c were converted into biimidazole hydrazide esters 10a-c. Compounds 7a-c and 10a-c were converted into a variety of derivatives. Full article
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<p>The synthesis of compounds <b>1 - 9a-c.</b></p> Full article ">Figure 2
<p>The synthesis of compounds <b>10(a-c) – 15(a-c)</b>.</p> Full article ">
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Article
Novel Biodegradable Polyesters. Synthesis and Application as Drug Carriers for the Preparation of Raloxifene HCl Loaded Nanoparticles
by Dimitrios Bikiaris, Vassilios Karavelidis and Evangelos Karavas
Molecules 2009, 14(7), 2410-2430; https://doi.org/10.3390/molecules14072410 - 7 Jul 2009
Cited by 48 | Viewed by 16992
Abstract
Raloxifene HCl is a drug with poor bioavailability and poor water solubility. Furthermore nο pharmaceutically acceptable organic solvent has been reported before to dilute the drug. It was observed that Raloxifene HCl can be diluted in a solvent mixture of acetone/water or ethanol/water. [...] Read more.
Raloxifene HCl is a drug with poor bioavailability and poor water solubility. Furthermore nο pharmaceutically acceptable organic solvent has been reported before to dilute the drug. It was observed that Raloxifene HCl can be diluted in a solvent mixture of acetone/water or ethanol/water. The aim of this study was to use biodegradable polymers in order to prepare Raloxifene HCl nanoparticles. For this purpose a series of novel biodegradable poly(ethylene succinate-co-propylene adipate) P(ESu-co-PAd) polyesters were synthesized following the polycondensation method and further, poly(ethylene succinate) (PESu) and poly(propylene adipate) (PPAd) were used. The prepared polyesters were characterized by intrinsic viscosity measurements, end group analysis, enzymatic hydrolysis, Nuclear Magnetic Resonance Spectroscopy (1Η-NMR and 13C-NMR) and Wide-angle X-ray Diffractometry (WAXD). The drug nanoparticles have been prepared by a variation of the co-precipitation method and were studied by Wide-angle X-ray Diffractometry (WAXD), FTIR spectrometry, light scattering size distribution, Scanning Electron Microscopy (SEM) and release behavior measurements. The interactions between the polymers and the drug seem to be limited, so the drug occurs in crystalline form in all nanoparticles. The size of the nanoparticles seems to be in the range of 150-350 nm, depending on the polymer that was used. The drug release depends on the melting point and degree of crystallinity of the polyesters used. An initial high release rate was recorded followed by very slow rates of controlled release. Full article
(This article belongs to the Special Issue Macromolecules Applied to Pharmaceutics)
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<p>Chemical structure of Raloxifene HCl.</p> Full article ">Figure 2
<p><sup>1</sup>H-NMR spectra of a) PESu, PPAd and b) their P(ESu-co-PAd) co-polymers.</p> Full article ">Figure 3
<p><sup>13</sup>C-NMR spectra of PESu, PPAd and their P(ESu-co-PAd) copolymers.</p> Full article ">Figure 4
<p>WAXD patterns of the PESu, PPAd and crystalline P(ESu-co-PAd) copolymers.</p> Full article ">Figure 5
<p>The percentage of mass loss vs time after enzymatic hydrolysis for P(ESu-co-PAd) copolymers.</p> Full article ">Figure 6
<p>HUVEC cells viability after incubation for 24 hours with different polymers and different polymer concentrations.</p> Full article ">Figure 7
<p>Particle size distribution of Raloxifene HCl loaded nanoparticles.</p> Full article ">Figure 8
<p>SEM micrographs of the Raloxifene loaded a) P(ESu-co-PAd) 70/30 copolymer and b) PPAd, nanoparticles.</p> Full article ">Figure 9
<p>Comparative WAXD patterns of Raloxifene HCl and the drug loaded nanoparticles.</p> Full article ">Figure 10
<p>Comparative FTIR spectra of Raloxifene HCl and the drug loaded nanoparticles.</p> Full article ">Figure 11
<p>Raloxifene HCl release profiles from the prepared nanoparticles of PESu, PPAd and P(ESu-co-PAd) 80/20 and 70/30 copolymers.</p> Full article ">Figure 12
<p>Synthetic route to P(ESu-co-PAd) copolymers preparation, via the two step polycondensation.</p> Full article ">
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Article
Transformations of Organic Molecules with F-TEDA-BF4 in Ionic Liquid Media
by Jasminka Pavlinac, Marko Zupan and Stojan Stavber
Molecules 2009, 14(7), 2394-2409; https://doi.org/10.3390/molecules14072394 - 6 Jul 2009
Cited by 14 | Viewed by 16301
Abstract
The transformations of organic molecules with F-TEDA-BF4 (1) were investigated in the hydrophilic ionic liquid (IL) 1-butyl-3-methyl-imidazolium tetrafluoroborate ([bmim][BF4], 2) and the hydrophobic IL 1-butyl-3-methyl-imidazolium hexafluorophosphate ([bmim][PF6], 3). The range of substrates included alkyl substituted phenols 4a-c, 9, [...] Read more.
The transformations of organic molecules with F-TEDA-BF4 (1) were investigated in the hydrophilic ionic liquid (IL) 1-butyl-3-methyl-imidazolium tetrafluoroborate ([bmim][BF4], 2) and the hydrophobic IL 1-butyl-3-methyl-imidazolium hexafluorophosphate ([bmim][PF6], 3). The range of substrates included alkyl substituted phenols 4a-c, 9, 13, 1,1-diphenylethene (15), alkyl aryl ketones 19-22, aldehydes 23-25 and methoxy-substituted benzene derivatives 26-30. The evaluation of the outcome of reactions performed in IL media in comparison to those of the corresponding reactions in conventional organic solvents revealed that the transformations in IL are less efficient and selective. The effect of the presence of a nucleophile (MeOH, H2O, MeCN) on the course of reaction was also studied. Full article
(This article belongs to the Collection Ionic Liquids)
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<p>Comparison of product distribution obtained in reaction of 4-<span class="html-italic">i</span>-propyl phenol (<b>4b</b>) or 4-<span class="html-italic">t</span>-butyl phenol (<b>4c</b>) with F-TEDA-BF<sub>4</sub> in ILs and organic solvents<sup>a</sup>.</p> Full article ">Figure 2
<p>Effect of the amount of nucleophile on the product distribution for fluorination of 1,1-diphenyl ethane (<b>15</b>) with F-TEDA-BF<sub>4</sub> in [bmim][BF<sub>4</sub>] and [bmim][PF<sub>6</sub>]<sup>a,b</sup>.</p> Full article ">Figure 3
<p>The mixture of products obtained in reaction of 1,3-dimethoxybenzene (<b>26</b>) or 1,3,5-trimethoxybenzene (<b>27</b>) with F-TEDA-BF<sub>4</sub> in the IL [bmim][BF<sub>4</sub>] or [bmim][PF<sub>6</sub>] (70 °C, 3-4 h).</p> Full article ">Figure 4
<p>Effect of reaction conditions on the course of transformation of organic molecules with F-TEDA-BF<sub>4</sub> in the presence of a nucleophile.</p> Full article ">Figure 5
<p>Transformation of 4-alkyl substituted phenols with F-TEDA-BF<sub>4</sub>.</p> Full article ">Figure 6
<p>Effect of reaction conditions on the reaction of 2,4,6-tri-t-butyl phenol (<b>9</b>) with F-TEDA-BF<sub>4</sub>.</p> Full article ">Figure 7
<p>Transformation of 3,4,5-trimethylphenol (<b>13</b>) with F-TEDA-BF<sub>4</sub> in the hydrophilic IL [bmim][BF<sub>4</sub>].</p> Full article ">Figure 8
<p>The selectivity of fluorotransformation of 1,1-diphenyl ethane (<b>15</b>) in reaction with F-TEDA-BF<sub>4</sub> in an IL.</p> Full article ">
342 KiB  
Review
Steroidal Lactones from Withania somnifera, an Ancient Plant for Novel Medicine
by Mohammad Hossein Mirjalili, Elisabeth Moyano, Mercedes Bonfill, Rosa M. Cusido and Javier Palazón
Molecules 2009, 14(7), 2373-2393; https://doi.org/10.3390/molecules14072373 - 3 Jul 2009
Cited by 452 | Viewed by 65489
Abstract
Withania somnifera, commonly known as Ashwagandha, is an important medicinal plant that has been used in Ayurvedic and indigenous medicine for over 3,000 years. In view of its varied therapeutic potential, it has also been the subject of considerable modern scientific attention. The [...] Read more.
Withania somnifera, commonly known as Ashwagandha, is an important medicinal plant that has been used in Ayurvedic and indigenous medicine for over 3,000 years. In view of its varied therapeutic potential, it has also been the subject of considerable modern scientific attention. The major chemical constituents of the Withania genus, the withanolides, are a group of naturally occurring C28-steroidal lactone triterpenoids built on an intact or rearranged ergostane framework, in which C-22 and C-26 are appropriately oxidized to form a six-membered lactone ring. In recent years, numerous pharmacological investigations have been carried out into the components of W. somnifera extracts. We present here an overview of the chemical structures of triterpenoid components and their biological activity, focusing on two novel activities, tumor inhibition and antiangiogenic properties of withaferin A and the effects of withanolide A on Alzheimer's disease. The most recent attempts in biotechnological production of withanolides are also discussed. Full article
(This article belongs to the Special Issue Triterpenes and Triterpenoids 2013)
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<p>The basic structure of withanolides.</p> Full article ">Figure 2
<p>Overview of the most important steps in the withanolide biosynthetic pathway.</p> Full article ">Figure 3
<p>Structure of withaferin A.</p> Full article ">Figure 4
<p>Different structures of withanolides.</p> Full article ">Figure 5
<p>Ashwagandhanolide, a new compound isolated from <span class="html-italic">W. somnifera</span><span class="html-italic">.</span></p> Full article ">Figure 6
<p>Different withanamides (A-I) isolated from <span class="html-italic">W. somnifera</span> fruits.</p> Full article ">
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Article
Salivary Aldehyde Dehydrogenase: Activity towards Aromatic Aldehydes and Comparison with Recombinant ALDH3A1
by Joanna Giebułtowicz, Renata Wolinowska, Anna Sztybor, Monika Pietrzak, Piotr Wroczyński and Jacek Wierzchowski
Molecules 2009, 14(7), 2363-2372; https://doi.org/10.3390/molecules14072363 - 2 Jul 2009
Cited by 27 | Viewed by 10439
Abstract
A series of aromatic aldehydes was examined as substrates for salivary aldehyde dehydrogenase (sALDH) and the recombinant ALDH3A1. Para-substituted benzaldehydes, cinnamic aldehyde and 2-naphthaldehydes were found to be excellent substrates, and kinetic parameters for both salivary and recombinant ALDH were nearly identical. It [...] Read more.
A series of aromatic aldehydes was examined as substrates for salivary aldehyde dehydrogenase (sALDH) and the recombinant ALDH3A1. Para-substituted benzaldehydes, cinnamic aldehyde and 2-naphthaldehydes were found to be excellent substrates, and kinetic parameters for both salivary and recombinant ALDH were nearly identical. It was demonstrated that for the fluorogenic naphthaldehydes the only produced reaction product after incubation in saliva is the carboxylate. Full article
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<p>HPLC elution profiles for oxidation of aromatic aldehydes with salivary ALDH, recorded with fluorimetric detector at 360 nm, with excitation at 315 nm. Reaction time was 5 (lowest curve), 10, 15 and 20 minutes (----).</p> Full article ">Figure 2
<p>Reaction progress curves, recorded fluorimetrically, for enzymatic oxidation of 2-naphthaldehde (left) and MONAL (right) with the recombinant ALDH3A1 as catalyst. Initial naphthaldehyde concentrations were 5, 2 and 1 μM. Concentration of NAD<sup>+</sup> was 100 μM.</p> Full article ">Figure 3
<p>The Lineweaver-Burk plot for the enzymatic oxidation of 2 μM MONAL catalyzed by the recombinant ALDH3A1. Rates were obtained by numerical differentiation of the progress curve from <a href="#molecules-14-02363-f002" class="html-fig">Fig. 2</a>. The fitted K<sub>m</sub> is 0.16 μM.</p> Full article ">Figure 4
<p>SDS/PAGE of recombinant ALDH3A1 after purification: lane 1, PageRuler (Fermantas) molecular mass marker proteins (from bottom to top: 26, 34, 43, 55, 72, 95, 130, 170 kDa); lane 2, solution from the first elution; lane 3, solution from the second elution; lane 4, eluate after dialysis. The gel was stained with Coomassie Brilliant Blue.</p> Full article ">Figure 5
<p>Enzymatic oxidation of aryl aldehydes, catalyzed by ALDH.</p> Full article ">
138 KiB  
Article
The Reaction of 4,5-Dichloro-1,2,3-dithiazolium Chloride with Sulfimides: A New Synthesis of N-Aryl-1,2,3-dithiazolimines
by Andreas S. Kalogirou and Panayiotis A. Koutentis
Molecules 2009, 14(7), 2356-2362; https://doi.org/10.3390/molecules14072356 - 2 Jul 2009
Cited by 6 | Viewed by 11802
Abstract
N-Aryl-S,S-dimethylsulfimides 3(Ar = 4-NO2C6H4), 4 (Ar = Ph) and 5 (Ar = 4-Tol)react with Appel salt 1 to give the corresponding N-aryl-(4-chloro-5H-1,2,3-dithiazolylidene)benzenamines 8 (Ar = 4-NO2C6 [...] Read more.
N-Aryl-S,S-dimethylsulfimides 3(Ar = 4-NO2C6H4), 4 (Ar = Ph) and 5 (Ar = 4-Tol)react with Appel salt 1 to give the corresponding N-aryl-(4-chloro-5H-1,2,3-dithiazolylidene)benzenamines 8 (Ar = 4-NO2C6H4), 9 (Ar = Ph) and 10 (Ar = 4-Tol) in 84, 94 and 87% yields, respectively. The reaction proceeds in the absence of base and a proposed reaction mechanism is given. Full article
(This article belongs to the Special Issue Advances in Heterocyclic Chemistry)
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<p>The classical reaction of anilines with Appel salt <b>1</b> to afford dithiazolimines <b>2</b>.</p> Full article ">Figure 2
<p>Proposed reaction mechanism for the reaction of sulfimide with 4,5-dichloro-1,2,3-dithiazolium chloride <b>1</b>.</p> Full article ">
260 KiB  
Article
A New Synthetic Compound, 2-OH, Enhances Interleukin-2 and Interferon-γ Gene Expression in Human Peripheral Blood Mononuclear Cells
by Shiu-Huey Chou, Shang-Shing P. Chou, Yih-Fong Liew, Jyh-Yih Leu, Su-Jane Wang, Rwei-Fen S. Huang, Woan-Fang Tzeng and Yuh-Chi Kuo
Molecules 2009, 14(7), 2345-2355; https://doi.org/10.3390/molecules14072345 - 2 Jul 2009
Cited by 7 | Viewed by 12604
Abstract
A new synthetic compound, 6-hydroxy-2-tosylisoquinolin-1(2H)-one (2-OH), was selected for immunopharmacological activity tests. The effects of 2-OH on human peripheral blood mononuclear cell (PBMC) proliferation were determined by tritiated thymidine uptake. Compared to phytohemagglutinin (PHA; 5 μg/mL) stimulation, 2-OH significantly enhanced PBMC [...] Read more.
A new synthetic compound, 6-hydroxy-2-tosylisoquinolin-1(2H)-one (2-OH), was selected for immunopharmacological activity tests. The effects of 2-OH on human peripheral blood mononuclear cell (PBMC) proliferation were determined by tritiated thymidine uptake. Compared to phytohemagglutinin (PHA; 5 μg/mL) stimulation, 2-OH significantly enhanced PBMC proliferation in a dose-dependent manner. The 50% enhancement activity (EC50) for 2-OH was 4.4±0.1 μM. In addition, effects of 2-OH on interleukin-2 (IL-2) and interferon-γ (IFN-γ) production in PBMC were determined by enzyme immunoassay. Results demonstrated that 2-OH stimulated IL-2 and IFN-γ production in PBMC. Data from reverse transcription-polymerase chain reaction (RT-PCR) and real-time PCR indicated that IL-2 and IFN-γ mRNA expression in PBMC could be induced by 2-OH. Therefore, 2-OH enhanced IL-2 and IFN-γ production in PBMC by modulation their gene expression. We suggest that 2-OH may be an immunomodulatory agent. Full article
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<p>The structure of <b>2-OH</b> (C<sub>16</sub>H<sub>13</sub>NO<sub>4</sub>S; M.W. 315).</p> Full article ">Figure 2
<p>Effects of <b>2-OH</b> on PBMC proliferation. PBMC (2×10<sup>5</sup>/well) were treated with 0.1% DMSO (control), PHA (5 µg/mL) or indicated concentrations of <b>2-OH</b> (1.5, 3.13, 6.25, 12.5, and 25 μM) for three days. The proliferation of cells were detected by tritiated thymidine uptake. After a 16 hr incubation, the cells were harvested by an automatic harvester then radioactivity was measured by a scintillation counting. Each bar represents the mean±S.D. of three independent experiments with PBMC from different individuals. *P &lt; 0.05, **P&lt; 0.01, as compared with control group.</p> Full article ">Figure 3
<p>The IL-2 and IFN-γ production in PBMC cultures treated with <b>2-OH</b>. PBMC (2×10<sup>5</sup>/well) were treated by 0.1% DMSO (control), PHA (5 µg/mL) or indicated concentrations of <b>2-OH</b> (1.5, 3.13, 6.25, 12.5, and 25 μM) for three days. Then the cell supernatants were collected and (A) IL-2 and (B) IFN-γ concentrations were determined by EIA. Each bar is the mean±S.D. of three independent experiments with PBMC from different individuals. *P &lt; 0.05, **P&lt; 0.01, ***P&lt; 0.001, as compared with control group.</p> Full article ">Figure 4
<p>Effects of <b>2-OH</b> on: (A) IL-2 and (B) IFN-γ mRNA expression in PBMC, as detected with RT-PCR. PBMC (5 x 10<sup>6</sup>) were cultured with PHA (5 µg/mL) or 6.25 and 25 μM <b>2-OH</b> for 18 hr. The total cellular RNA was isolated from PBMC and aliquots of RNA (1 μg) were reverse-transcribed for synthesis of cDNA. PCR was done as described in Materials and Methods. Following the reaction, the amplified product was taken out of the tubes and run on 2% agarose gel. Lane 1: Control (0.1% DMSO), Lane 2: PHA, Lane 3: 6.25 μM <b>2-OH</b>, Lane 4: 12.5 μM <b>2-OH</b>. Each band was quantitated using laser scanning densitometer SLR-2D/1D (Biomed Instruments Inc., Fullerton, CA, USA). The ratio of IL-2 or IFN-γ mRNA to GAPDH mRNA was calculated. Each bar is the mean±S.D. of three independent experiments with PBMC from different individuals. **P &lt; 0.01, ***P &lt; 0.001, as compared with control group.</p> Full article ">
54 KiB  
Review
Selenium and the Methionine Sulfoxide Reductase System
by Derek B. Oien and Jackob Moskovitz
Molecules 2009, 14(7), 2337-2344; https://doi.org/10.3390/molecules14072337 - 1 Jul 2009
Cited by 13 | Viewed by 13572
Abstract
Selenium is a chemical element participating in the synthesis of selenocysteine residues that play a pivotal role in the enzymatic activity efficiency of selenoproteines. The methionine sulfoxide reductase (Msr) system that reduces methionine sulfoxide (MetO) to methionine comprises the selenoprotein MsrB (MsrB1) and [...] Read more.
Selenium is a chemical element participating in the synthesis of selenocysteine residues that play a pivotal role in the enzymatic activity efficiency of selenoproteines. The methionine sulfoxide reductase (Msr) system that reduces methionine sulfoxide (MetO) to methionine comprises the selenoprotein MsrB (MsrB1) and the non-selenoprotein MsrA, which reduce the R- and the S- forms of MetO, respectively. The effects of a selenium deficient (SD) diet, which was administrated to wild type (WT) and MsrA knockout mice (MsrA-/-), on the expression and function of Msr-related proteins are examined and discussed. Additionally, new data about the levels of selenium in brain, liver, and kidneys of WT and MsrA-/- mice are presented and discussed. Full article
(This article belongs to the Special Issue Selenium and Tellurium Chemistry)
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<p>Selenium content in wild type and <span class="html-italic">MsrA<sup>-</sup>/<sup>-</sup></span> mice. The selenium content (ppm) was measured by the relevant NAA method [<a href="#B20-molecules-14-02337" class="html-bibr">20</a>,<a href="#B21-molecules-14-02337" class="html-bibr">21</a>] in brain, liver and kidney using the same dry mass tissue from each organ. The quality control Sample was NIST SRM 1577 Bovine Liver (certified Se concentration = 1.1 +/- 0.1 ppm). The symbol * represents significant difference (<span class="html-italic">p</span>=0.05; <span class="html-italic">t-test</span>) between the averaged values of 3 independent experiments determining selenium content in tissues of wild type and <span class="html-italic">MsrA<sup>-</sup>/<sup>- </sup></span>mice (significantly lower selenium levels were observed in brain (-23%; <span class="html-italic">p</span>=0.05) and liver (-8%; <span class="html-italic">p</span>=0.043) of <span class="html-italic">MsrA<sup>-</sup>/<sup>- </sup></span>when compared with WT mice, respectively). Note: in the <span class="html-italic">MsrA<sup>-</sup>/<sup>- </sup></span>liver all measurements gave the same value; thus, no standard deviation is given.</p> Full article ">
537 KiB  
Review
Pentavalent Antimonials: New Perspectives for Old Drugs
by Frédéric Frézard, Cynthia Demicheli and Raul R. Ribeiro
Molecules 2009, 14(7), 2317-2336; https://doi.org/10.3390/molecules14072317 - 30 Jun 2009
Cited by 357 | Viewed by 31192
Abstract
Pentavalent antimonials, including meglumine antimoniate and sodium stibogluconate, have been used for more than half a century in the therapy of the parasitic disease leishmaniasis. Even though antimonials are still the first-line drugs, they exhibit several limitations, including severe side effects, the need [...] Read more.
Pentavalent antimonials, including meglumine antimoniate and sodium stibogluconate, have been used for more than half a century in the therapy of the parasitic disease leishmaniasis. Even though antimonials are still the first-line drugs, they exhibit several limitations, including severe side effects, the need for daily parenteral administration and drug resistance. The molecular structure of antimonials, their metabolism and mechanism of action are still being investigated. Some recent studies suggest that pentavalent antimony acts as a prodrug that is converted to active and more toxic trivalent antimony. Other works support the direct involvement of pentavalent antimony. Recent data suggest that the biomolecules, thiols and ribonucleosides, may mediate the actions of these drugs. This review will summarize the progress to date on the chemistry and biochemistry of pentavalent antimony. It will also present the most recent works being done to improve antimonial chemotherapy. These works include the development of simple synthetic methods for pentavalent antimonials, liposome-based formulations for targeting the Leishmania parasites responsible for visceral leishmaniasis and cyclodextrin-based formulations to promote the oral delivery of antimony. Full article
(This article belongs to the Special Issue Neglected Diseases: Medicinal Chemistry and Natural Product Chemistry)
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<p>Proposed structural formula for 364 Da and 365 Da ions identified by ESI(-)-MS in aqueous solutions of meglumine antimoniate and stibogluconate, respectively. Adapted from Ref. [<a href="#B23-molecules-14-02317" class="html-bibr">23</a>].</p> Full article ">Figure 2
<p>Two main models proposed for the mechanism of action of pentavalent antimonials against leishmaniasis. According to the “Prodrug model”, Sb(V) is reduced to Sb(III) in order to exert antileishmanial activity. According to the “Active Sb(V) model”, Sb(V) exhibits intrinsic antileishmanial activity.</p> Full article ">Figure 3
<p>Processes used for the preparation of meglumine antimoniate-containing liposomes of different size. Adapted from Ref. [<a href="#B84-molecules-14-02317" class="html-bibr">84</a>,<a href="#B85-molecules-14-02317" class="html-bibr">85</a>,<a href="#B86-molecules-14-02317" class="html-bibr">86</a>,<a href="#B87-molecules-14-02317" class="html-bibr">87</a>].</p> Full article ">Figure 4
<p>Influence of liposome encapsulation and of vesicle mean diameter on antimony level in the bone marrow of infected dogs, 96 h after intravenous bolus injection of meglumine antimoniate. Small liposomes (mean vesicle diameter of 400 nm) were given at 4 mg Sb/kg of body weight (n = 5). Large liposomes (mean vesicle diameter of 1,200 nm) were given at 5.5 mg Sb/kg of body weight (n = 10). Meglumine antimoniate was given at 100 mg Sb/kg of body weight (n = 5). Data are given as means ± standard deviation. *<span class="html-italic">P</span> &lt;0.001 for One-way ANOVA followed by Bonferroni post-test. Adapted from Ref. [<a href="#B84-molecules-14-02317" class="html-bibr">84</a>].</p> Full article ">Figure 5
<p>Model proposed for the mechanisms involved in the enhanced absorption of Sb from oral meglumine antimoniate/β-CD composition. The meglumine antimoniate/β-CD nanoassemblies comprising high-molecular weight meglumine antimoniate/β-CD complexes, such as NMG-Sb-β-CD-Sb-NMG species, migrate along the gastrointestinal tract. These nanoassemblies then slowly release meglumine antimoniate in the form of 1:1 Sb-NMG complex which permeates by simple diffusion across the gastrointestinal epithelium. β-CD continue migrating up to the colon where it is degraded. Adapted from Ref. [<a href="#B102-molecules-14-02317" class="html-bibr">102</a>].</p> Full article ">
268 KiB  
Article
Synthesis and Antitumor Evaluation of Novel Bis-Triaziquone Derivatives
by Cheng Hua Huang, Hsien-Shou Kuo, Jia-Wen Liu and Yuh-Ling Lin
Molecules 2009, 14(7), 2306-2316; https://doi.org/10.3390/molecules14072306 - 29 Jun 2009
Cited by 13 | Viewed by 14743
Abstract
Aziridine-containing compounds have been of interest as anticancer agents since late 1970s. The design, synthesis and study of triaziquone (TZQ) analogues with the aim of obtaining compounds with enhanced efficacy and reduced toxicity are an ongoing research effort in our group. A series [...] Read more.
Aziridine-containing compounds have been of interest as anticancer agents since late 1970s. The design, synthesis and study of triaziquone (TZQ) analogues with the aim of obtaining compounds with enhanced efficacy and reduced toxicity are an ongoing research effort in our group. A series of bis-type TZQ derivatives has been prepared and their cytotoxic activities were investigated. The cytotoxicity of these bis-type TZQ derivatives were tested on three cancer lines, including breast cancer (BC-M1), oral cancer (OEC-M1), larynx epidermal cancer (Hep2) and one normal skin fibroblast (SF). Most of these synthetic derivatives displayed significant cytotoxic activities against human carcinoma cell lines, but weak activities against SF. Among tested analogues the bis-type TZQ derivative 1a showed lethal effects on larynx epidermal carcinoma cells (Hep2), with an LC50 value of 2.02 mM, and also weak cytotoxic activity against SF cells with an LC50 value over 10 mM for 24 hr treatment. Comparing the viability of normal fibroblast cells treated with compound 1a and TZQ, the LC50 value of the latter was 2.52 mM, indicating more toxicity than compound 1a. This significantly decreased cytotoxicity of compound 1a towards normal SF cells, while still maintaining the anticancer activity towards Hep2 cells is an interesting feature. Among the seven compounds synthesized, compound 1c has similar toxicity effects on the three cancer cell lines and SF normal cells as the TZQ monomer. Full article
(This article belongs to the Special Issue Quinones and Hydroxyquinones. Target Molecules and Building Blocks in Organic Synthesis)
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<p>Compound <b>1a</b> and TZQ inhibited the proliferation of cell lines Hep 2 (A) and SF (B) that were seeded for 18 hr before the addition of two compounds with various concentrations. The MTT assay was used to determine the cell viability after an additional 24 hr of culture. Data were from triplet wells and are representative of three separate experiments.</p> Full article ">Figure 2
<p>Compounds <b>1b</b> to <b>1f</b> inhibited the proliferation of cell lines Hep 2 (A) and SF (B), 1a to 1f compounds and TZQ inhibited the proliferation of cell lines OEC-M1 (C) and BC-M1 (D) that were seeded for 18 hr before the addition of two compounds with various concentrations. The MTT assay was used to determine the cell viability after an additional 24 hr of culture. Data were from triplet wells and are representative of three separate experiments.</p> Full article ">Figure 3
<p>The chemical synthesis of bis-triaziquone derivatives <b>1a-g</b> and structure of TZQ.</p> Full article ">
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