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Molecules, Volume 15, Issue 10 (October 2010) – 57 articles , Pages 6678-7508

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502 KiB  
Article
Synthesis of New Azo Compounds Based on N-(4-Hydroxypheneyl)maleimide and N-(4-Methylpheneyl)maleimide
by Issam Ahmed Mohammed and Asniza Mustapha
Molecules 2010, 15(10), 7498-7508; https://doi.org/10.3390/molecules15107498 - 25 Oct 2010
Cited by 54 | Viewed by 11344
Abstract
Maleic anhydride was reacted with p-aminophenol and p-toluidine in the presence of di-phosphorus pentoxide (P2O5) as a catalyst to produce two compounds: N-(4-hydroxy-phenyl)maleimide (I) and N-(4-methylphenyl)maleimide (II). The new azo compounds [...] Read more.
Maleic anhydride was reacted with p-aminophenol and p-toluidine in the presence of di-phosphorus pentoxide (P2O5) as a catalyst to produce two compounds: N-(4-hydroxy-phenyl)maleimide (I) and N-(4-methylphenyl)maleimide (II). The new azo compounds I(a-c) and II(a-c) were prepared by the reaction of I and II with three different aromatic amines, namely aniline, p-aminophenol and p-toluidine. The structures of these compounds were confirmed by CHN, FT-IR, 1H-NMR, 13C-NMR, mass spectrum and UV/Vis spectroscopy. Full article
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Figure 1
<p>FT-IR spectrum of compound <b>Ia</b>.</p> Full article ">Figure 2
<p><sup>1</sup>H-NMR spectra of (A) compound <b>I</b> and (B) compound <b>Ia </b>in CD<sub>3</sub>OD.</p> Full article ">Figure 3
<p><sup>13</sup>C-NMR spectra of (A) compound <b>I</b> and (B) compound <b>Ia </b>in CD<sub>3</sub>OD.</p> Full article ">Figure 4
<p>Mass spectrum of compound <b>Ia</b>.</p> Full article ">Figure 5
<p>Synthesis of N-(4-hydroxypheneyl)maleimide (<b>I</b>), N-(4-methylpheneyl)maleimide (<b>II</b>), <b>I(a-c) </b>and<b> II(a-c)</b>.</p> Full article ">
224 KiB  
Article
Lead Contamination in Selected Foods from Riyadh City Market and Estimation of the Daily Intake
by Zeid A. Al Othman
Molecules 2010, 15(10), 7482-7497; https://doi.org/10.3390/molecules15107482 - 25 Oct 2010
Cited by 39 | Viewed by 9351
Abstract
This study was carried out to determine lead contamination in 104 of the representative food items in the Saudi diet and to estimate the dietary lead intake of Saudi Arabians. Three samples of each selected food items were purchased from the local markets [...] Read more.
This study was carried out to determine lead contamination in 104 of the representative food items in the Saudi diet and to estimate the dietary lead intake of Saudi Arabians. Three samples of each selected food items were purchased from the local markets of Riyadh city, the capital of Saudi Arabia. Each pooled sample was analyzed in triplicate by ICP-AES after thorough homogenization. Sweets (0.011–0.199 μg/g), vegetables (0.002–0.195 μg/g), legumes (0.014–0.094 μg/g), eggs (0.079 μg/g), meat and meat products (0.013–0.068 μg/g) were the richest sources of lead. Considering the amounts of each food consumed, the major food sources of lead intake for Saudi can be arranged as follows: vegetables (25.4%), cereal and cereal products (24.2%), beverages (9.7%) sweets (8.2%), legumes (7.4%), fruits (5.4%) milk and milk products (5.1%). The daily intake of lead was calculated taking into account the concentration of this element in the edible part of the daily consumption data which were derived from two sources, (a) the KSA food sheet provided by the Food and Agriculture Organization (FAO) and (b) from questionnaires distributed among 300 families in Riyadh city. The results showed that the daily intakes of lead according to the two sources are 22.7 and 24.5 μg/person/day respectively, which are lower than that mentioned by The Joint Expert Committee on Food Additives (JECFA), whereas it is comprabale with that of other countries. Full article
117 KiB  
Article
Synthesis of Novel 1-[(2,6-Dichloro-4-trifluoromethyl)phenyl]-3-aryl-1H-pyrazole-4-carbaldehydes
by Huanan Hu, Changhua Ge, Lisheng Ding and Anjiang Zhang
Molecules 2010, 15(10), 7472-7481; https://doi.org/10.3390/molecules15107472 - 25 Oct 2010
Cited by 19 | Viewed by 7173
Abstract
A series of novel 1-[(2,6-dichloro-4-trifluoromethyl)phenyl]-3-aryl-1H-pyrazole-4-carbaldehydes 6a-i were synthesized using the Vilsmeier-Haack reagent. The structures of all the title compounds have been confirmed by elemental analysis, 1H-NMR and 13C-NMR and in addition, the structure of intermediate 5b was investigated by X-ray crystallography. Full article
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<p>ORTEP drawing of the compound <b>5b</b> showing the atom numbering scheme.</p> Full article ">Figure 2
<p>Synthesis of phenylhydrazine <b>3</b>.</p> Full article ">Figure 3
<p>Synthesis of phenylhydrazones <b>5</b>.</p> Full article ">Figure 4
<p>Synthesis of 1<span class="html-italic">H</span>-pyrazole-4-carbaldehydes <b>6</b>.</p> Full article ">
137 KiB  
Article
A New Natural Ceramide from Trollius chinensis Bunge
by Ru-Feng Wang, Rui-Ning Liu, Tong Zhang and Tao Wu
Molecules 2010, 15(10), 7467-7471; https://doi.org/10.3390/molecules15107467 - 25 Oct 2010
Cited by 14 | Viewed by 7741
Abstract
A new natural product named trolliamide was isolated from Trollius chinensis Bunge. Its structure was determined as 2-hydroxy-tetracosanoic acid(2,3-dihydroxy-1-hydroxymethyl-heptadec-7-enyl)-amide by spectroscopic methods, including UV, IR, MS and NMR. This is the first report of a ceramide isolated from Trollius chinensis. Full article
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<p>The structure of trolliamide.</p> Full article ">
181 KiB  
Article
Creation of a Databank for Content of Antioxidants in Food Products by an Amperometric Method
by Yakov I. Yashin, Boris V. Nemzer, Vadim Yu. Ryzhnev, Alexandr Ya. Yashin, Nina I. Chernousova and Polina A. Fedina
Molecules 2010, 15(10), 7450-7466; https://doi.org/10.3390/molecules15107450 - 22 Oct 2010
Cited by 27 | Viewed by 11074
Abstract
Oxidative stress, i.e. excessive content of reactionary, oxygen, and nitrogen compounds (ROAC), including free radicals, is one of the causes of various dangerous diseases as well as premature aging. The adverse effect of free radicals can be neutralized by antioxidants. In order to [...] Read more.
Oxidative stress, i.e. excessive content of reactionary, oxygen, and nitrogen compounds (ROAC), including free radicals, is one of the causes of various dangerous diseases as well as premature aging. The adverse effect of free radicals can be neutralized by antioxidants. In order to carry out antioxidant therapy, one needs to know the contents of antioxidants in food products. We have created the databank for the contents of antioxidants in 1,140 food products, beverages, etc. Apart from water-soluble antioxidants, fat-soluble antioxidants in dairy and fish products, cacao, chocolate, nuts etc. were determined for the first time using an amperometric method. Full article
244 KiB  
Article
Prenylated Xanthones from the Bark of Garcinia xanthochymus and Their 1,1-Diphenyl-2-picrylhydrazyl (DPPH) Radical Scavenging Activities
by Yu Chen, Hua Fan, Guang-zhong Yang, Yan Jiang, Fang-fang Zhong and Hong-wu He
Molecules 2010, 15(10), 7438-7449; https://doi.org/10.3390/molecules15107438 - 22 Oct 2010
Cited by 27 | Viewed by 10884
Abstract
Garcinia xanthochymus has been widely used in traditional Chinese medicine for expelling worms and removing food toxins. Bioassay-guided fractionation of an EtOAc-soluble extract of G. xanthochymus stem bark led to the isolation of six new xanthones. Their structures were elucidated by spectroscopic methods, [...] Read more.
Garcinia xanthochymus has been widely used in traditional Chinese medicine for expelling worms and removing food toxins. Bioassay-guided fractionation of an EtOAc-soluble extract of G. xanthochymus stem bark led to the isolation of six new xanthones. Their structures were elucidated by spectroscopic methods, especially 2D-NMR techniques. Free-radical-scavenging activities of the isolated compounds were elucidated through DPPH method. Most of the isolated compounds showed considerable free radical scavenging activity on DPPH assay. Compound 1 exhibited effective antioxidant scavenging activity against DPPH radical with an IC50 value of 19.64 μM, and compound 6 showed the lowest activity among all the tested molecules, with an IC50 value of 66.88 μM. These findings support the notion that the plant genus Garcinia is a good source of bioactive compounds. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>Structures of compounds <b>1</b>-<b>6</b>.</p> Full article ">Figure 2
<p>Significant HMBC correlations of compound <b>1</b> and <b>3</b>.</p> Full article ">
226 KiB  
Article
One-Pot Synthesis of 2,3,4-Triarylquinolines via Suzuki-Miyaura Cross-Coupling of 2-Aryl-4-chloro-3-iodoquinolines with Arylboronic Acids
by Malose Jack Mphahlele and Mamasegare Mabel Mphahlele
Molecules 2010, 15(10), 7423-7437; https://doi.org/10.3390/molecules15107423 - 22 Oct 2010
Cited by 10 | Viewed by 6139
Abstract
Palladium–catalyzed Suzuki cross-coupling of 2-aryl-4-chloro-3-iodoquinolines with excess arylboronic acids (2.5 equiv.) in the presence of tricyclohexylphosphine afforded the 2,3,4-triarylquinolines in one-pot operation. The incipient 2,3-diaryl-4-chloroquinolines were also prepared and transformed to the primary 4-amino-2,3-diarylquinolines and 2,3-diarylquinolin-4(1H)-ones. Full article
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<p>X-ray crystal structure of 2,3,4-tris(4-fluorophenyl)quinoline <b>3f</b> showing crystallographic numbering. For clarity, hydrogen atoms are not labelled.</p> Full article ">Scheme 1
<p>Suzuki-Miyaura cross-coupling of 2-aryl-4-chloro-3-iodoquinolines.</p> Full article ">Scheme 2
<p>Successive C-3 arylation and amination of <b>1</b>.</p> Full article ">Scheme 3
<p>Hydrolysis of <b>2</b> to NH-4-oxo derivatives <b>5</b>.</p> Full article ">
199 KiB  
Article
Evaluation on Anti-hepatitis Viral Activity of Vitis vinifer L
by Tao Liu, Jun Zhao, Haibo Li and Long Ma
Molecules 2010, 15(10), 7415-7422; https://doi.org/10.3390/molecules15107415 - 22 Oct 2010
Cited by 14 | Viewed by 9084
Abstract
Suosuo grape (Vitis vinifer L) is traditionally used as a therapeutic agent for measles and hepatitis by the ethnic Uighurs. This work aimed to investigate the anti-HBV effect of total triterpene (VTT), total flavonoids (VTF) and total polysaccharides (VTP) from Suosuo grape, [...] Read more.
Suosuo grape (Vitis vinifer L) is traditionally used as a therapeutic agent for measles and hepatitis by the ethnic Uighurs. This work aimed to investigate the anti-HBV effect of total triterpene (VTT), total flavonoids (VTF) and total polysaccharides (VTP) from Suosuo grape, and their synergistic effects were also tested. The viral antigens of cellular secretion, HBsAg and HBeAg, were determined by enzyme linked immunosorbent assay (ELISA).The quantity of HBV-DNA released in the supernatant was assayed by real-time PCR. It was found that it effectively suppressed the secretion of HBsAg and HBeAg from HepG2.2.15 cells in a dose-dependent manner, as well as the HBV DNA. The results of orthogonal design experiment showed that the combination of VTT 20 μg/mL, VTF 50 μg/mL and VTP 50 μg/mL had the best optimistic inhibitory effects on HBeAg secretion. Full article
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<p>Inhibitory effect of VTP, VTT, VTF and 3-TC on HBsAg and HBeAg secretion.</p> Full article ">
292 KiB  
Article
The Pharmacological Effects of Morroniside and Loganin Isolated from Liuweidihuang Wan, on MC3T3-E1 Cells
by Manyu Li, Wei Wang, Ping Wang, Kun Yang, Hui Sun and Xijun Wang
Molecules 2010, 15(10), 7403-7414; https://doi.org/10.3390/molecules15107403 - 21 Oct 2010
Cited by 54 | Viewed by 10845
Abstract
Liuweidihuang Wan (LW), initially a well-known formula for curing “wu chi wu ruan”, is commonly used nowadays for clinical treatment of Postmenopausal Osteoporosis (PO), but the identity of the effective substance(s) remains unclear. The present study was designed to evaluate the effects of [...] Read more.
Liuweidihuang Wan (LW), initially a well-known formula for curing “wu chi wu ruan”, is commonly used nowadays for clinical treatment of Postmenopausal Osteoporosis (PO), but the identity of the effective substance(s) remains unclear. The present study was designed to evaluate the effects of morroniside and loganin isolated from LW on the proliferation, differentiation and apoptosis of MC3T3-E1 cells, as well as the possible mechanism of action. Morroniside and loganin had no effects on the proliferation of MC3T3-E1 cells, but both susbtances could improve the activity of alkaline phosphatase (ALP), and increase the contents of collagen type I and osteocalcin. Simultaneously, the mRNA expression of caspase-3, capase-9, RANKL was down-regulated and that of bcl-2 was up-regulated, which partially explains the anti-osteoporosis mechanism in MC3T3-E1 cells. In conclusion, morroniside and loganin may directly promote the differentiation and inhibit the apoptosis of MC3T3-E1 cells, and accordingly indirectly reduce bone resorption, which makes them promising natural drugs leads for treating PO in the near future. Full article
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<p>The effects of morronside and loganin on the proliferation of MC3T3-E1 cells. Cells were cultured with medium containing different concentrations (1, 10, 100 μg/mL) of the two constituents for 96 h and the viability of cells was measured by MTT method; <b>B:</b> The activity of ALP in MC3T3-E1 cells; <b>C:</b> The contents of osteocalcin in MC3T3-E1 cells; <b>D:</b> The contents of collagen type I in MC3T3-E1 cells.</p> Full article ">Figure 1 Cont.
<p>The effects of morronside and loganin on the proliferation of MC3T3-E1 cells. Cells were cultured with medium containing different concentrations (1, 10, 100 μg/mL) of the two constituents for 96 h and the viability of cells was measured by MTT method; <b>B:</b> The activity of ALP in MC3T3-E1 cells; <b>C:</b> The contents of osteocalcin in MC3T3-E1 cells; <b>D:</b> The contents of collagen type I in MC3T3-E1 cells.</p> Full article ">Figure 2
<p>The amounts of caspase-3 mRNA in MC3T3-E1 cells; <b>B:</b> The amounts of caspase-9 mRNA in MC3T3-E1 cells; <b>C:</b> The amounts of bcl-2 mRNA in MC3T3-E1 cells; <b>D:</b> The amounts of RANKL mRNA in MC3T3-E1 cells.</p> Full article ">Figure 3
<p>The HPLC charts of LW and the marked peaks of morronside and loganin.</p> Full article ">Figure 4
<p>The molecular mechanism of morroniside and loganin on treating osteoporosis.</p> Full article ">
304 KiB  
Article
Antibacterial Activity of Phytochemicals Isolated from Atractylodes japonica against Methicillin-Resistant Staphylococcus aureus
by Seung-Il Jeong, Seon-Young Kim, Sang-Jun Kim, Byung-Soon Hwang, Tae-Ho Kwon, Kang-Yeol Yu, Seung-Ho Hang, Koji Suzuki and Kang-Ju Kim
Molecules 2010, 15(10), 7395-7402; https://doi.org/10.3390/molecules15107395 - 21 Oct 2010
Cited by 34 | Viewed by 10761
Abstract
Methicillin-resistant Staphylococcus aureus (MRSA) has been emerging worldwide as one of the most important problems in communities and hospitals. Therefore, new agents are needed to treat acute oral infections from MRSA. In this study, antibacterial compounds from the roots of Atractylodes japonica ( [...] Read more.
Methicillin-resistant Staphylococcus aureus (MRSA) has been emerging worldwide as one of the most important problems in communities and hospitals. Therefore, new agents are needed to treat acute oral infections from MRSA. In this study, antibacterial compounds from the roots of Atractylodes japonica (A. japonica) were isolated and characterized. The compounds were isolated from the root extracts using HPLC-piloted activity-guided fractionations. Four A. japonica compounds were isolated and identified as atractylenolide III (1), atractylenolide I (2), diacetylatractylodiol [(6E,12E)-tetradeca-6,12-diene-8,10-diyne-1,3-diol diacetate, TDEYA, 3). and (6E,12E)-tetradecadiene-8,10-diyne-1,3-diol (TDEA, 4), which was obtained by hydrolysis of TDEYA. The minimum inhibitory concentrations (MICs) was determined in the setting of clinical MRSA isolates. Compound 4 showed anti-MRSA activity with a MIC value of 4-32 μg/mL. The overall results provide promising baseline information for the potential use of the extract of A. japonica as well as some of the isolated compounds in the treatment of bacterial infections. Full article
(This article belongs to the Collection Bioactive Compounds)
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<p>Chemical structures of isolated compounds from roots of <span class="html-italic">A. japonica</span>: atractylenolide III (1); atractylenolide I (<b>2</b>); (6<span class="html-italic">E</span>, 12<span class="html-italic">E</span>)-tetradecadiene-8,10-diyne-1,3-diol diacetate (diacetylatractylodiol TDEYA, <b>3</b>); (6<span class="html-italic">E</span>, 12<span class="html-italic">E</span>)-tetradecadiene-8,10-diyne-1,3-diol (TDEA, <b>4</b>).</p> Full article ">Figure 2
<p>Smart HPLC chromatographic fingerprints of MeOH extract of <span class="html-italic">A. japonica</span>. The peaks marked with 2, 6 and 7 are atractylenolide III, atractylenolide I, (6<span class="html-italic">E</span>,12<span class="html-italic">E</span>)-teradecadiene-8,10-diyne-1,3-diol diacetate (diacetylatractylodiol, TDEYA), respectively. The separation conditions are described in the Smart HPLC chromatographic conditions.</p> Full article ">
212 KiB  
Article
Synthesis, Gastroprotective Effect and Cytotoxicity of New Amino Acid Diterpene Monoamides and Diamides
by Guillermo Schmeda-Hirschmann, Mariano Walter Pertino, Jaime A. Rodriguez, Francisco Monsalve, Daniel Droguett and Cristina Theoduloz
Molecules 2010, 15(10), 7378-7394; https://doi.org/10.3390/molecules15107378 - 21 Oct 2010
Cited by 7 | Viewed by 10656
Abstract
Following our studies on the gastroprotective effect and cytotoxicity of terpene derivatives, new amides were prepared from the diterpene 8(17)-labden-15,19-dioic acid (junicedric acid) and its 8(9)-en isomer with C-protected amino acids (amino acid esters). The new compounds were evaluated for their gastroprotective effect [...] Read more.
Following our studies on the gastroprotective effect and cytotoxicity of terpene derivatives, new amides were prepared from the diterpene 8(17)-labden-15,19-dioic acid (junicedric acid) and its 8(9)-en isomer with C-protected amino acids (amino acid esters). The new compounds were evaluated for their gastroprotective effect in the ethanol/HCl-induced gastric lesions model in mice, as well as for cytotoxicity using the following human cell lines: normal lung fibroblasts (MRC-5), gastric adenocarcinoma cells (AGS) and liver hepatocellular carcinoma (Hep G2). A dose-response experiment showed that at 25 mg/kg the C-15 leucyl and C-15,19-dileucylester amides of junicedric acid reduced gastric lesions by about 65.6 and 49.6%, respectively, with an effect comparable to lansoprazole at 20 mg/kg (79.3% lesion reduction). The comparison of the gastroprotective effect of 18 new amino acid ester amides was carried out at a single oral dose of 25 mg/kg. Several compounds presented a strong gastroprotective effect, reducing gastric lesions in the 70.9-87.8% range. The diprolyl derivative of junicedric acid, the most active product of this study (87.8% lesion reduction at 25 mg/kg) presented a cytotoxicity value comparable with that of the reference compound lansoprazole. The structure-activity relationships are discussed. Full article
(This article belongs to the Section Medicinal Chemistry)
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<p>General procedure to prepare C-19 amides from imbricatolic acid and acetoxyimbricatolic acid as well as from the 8(9)-en isomers.</p> Full article ">Figure 2
<p>General procedure to prepare monoamides and diamides from dicarboxylic labdane diterpenes.</p> Full article ">
667 KiB  
Article
Chemometric Studies on Natural Products as Potential Inhibitors of the NADH Oxidase from Trypanosoma cruzi Using the VolSurf Approach
by Luciana Scotti, Elizabeth Igne Ferreira, Marcelo Sobral da Silva and Marcus Tullius Scotti
Molecules 2010, 15(10), 7363-7377; https://doi.org/10.3390/molecules15107363 - 21 Oct 2010
Cited by 42 | Viewed by 11484
Abstract
Natural products have widespread biological activities, including inhibition of mitochondrial enzyme systems. Some of these activities, for example cytotoxicity, may be the result of alteration of cellular bioenergetics. Based on previous computer-aided drug design (CADD) studies and considering reported data on structure-activity relationships [...] Read more.
Natural products have widespread biological activities, including inhibition of mitochondrial enzyme systems. Some of these activities, for example cytotoxicity, may be the result of alteration of cellular bioenergetics. Based on previous computer-aided drug design (CADD) studies and considering reported data on structure-activity relationships (SAR), an assumption regarding the mechanism of action of natural products against parasitic infections involves the NADH-oxidase inhibition. In this study, chemometric tools, such as: Principal Component Analysis (PCA), Consensus PCA (CPCA), and partial least squares regression (PLS), were applied to a set of forty natural compounds, acting as NADH-oxidase inhibitors. The calculations were performed using the VolSurf+ program. The formalisms employed generated good exploratory and predictive results. The independent variables or descriptors having a hydrophobic profile were strongly correlated to the biological data. Full article
(This article belongs to the Special Issue Phenolics and Polyphenolics)
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<p>Geographic distribution of Chagas’ disease.</p> Full article ">Figure 2
<p>Chemical structure of flavones.</p> Full article ">Figure 3
<p>Plot of block weights considering PC or factor 1 and 2.</p> Full article ">Figure 4
<p>Scores plot from PCA, where active compounds, compounds having medium activity, and inactive compounds are represented as A, M, and I, respectively.</p> Full article ">Figure 5
<p>Plot of <span class="html-italic">r<sup>2</sup></span> and <span class="html-italic">q<sup>2</sup> versus</span> the number of latent variables (LV) considering the PLS models.</p> Full article ">Figure 6
<p>Discriminant PLS t1-t2 scores plot for the global model (A = active; I = inactive).</p> Full article ">Figure 7
<p>Coefficients plot generated from the selected PLS model.</p> Full article ">
184 KiB  
Article
Tetrabutylammonium Bromide Media Aza-Michael Addition of 1,2,3,6-Tetrahydrophthalimide to Symmetrical Fumaric Esters and Acrylic Esters under Solvent-Free Conditions
by Gholamhassan Imanzadeh, Farzaneh Ahmadi, Mohammadreza Zamanloo and Yagoub Mansoori
Molecules 2010, 15(10), 7353-7362; https://doi.org/10.3390/molecules15107353 - 21 Oct 2010
Cited by 19 | Viewed by 11069
Abstract
The aza-Michael addition of 1,2,3,6-tetrahydrophthalimide with symmetrical fumaric esters has been performed efficiently in a solvent-free system at 100 °C and using 1,4-diazabicyclo[2.2.2]octane (DABCO) as a base in the presence of tetrabutylammonium bromide (TBAB). The products were obtained in good to high yields [...] Read more.
The aza-Michael addition of 1,2,3,6-tetrahydrophthalimide with symmetrical fumaric esters has been performed efficiently in a solvent-free system at 100 °C and using 1,4-diazabicyclo[2.2.2]octane (DABCO) as a base in the presence of tetrabutylammonium bromide (TBAB). The products were obtained in good to high yields within 2.5-7.0 h. This reaction worked well on linear alkyl fumarates and was not effective with nonlinear alkyl fumarates. Although the reaction was also applicable to acrylates such as n-butyl acrylate, methacrylates and crotonates were not suitable Michael acceptors for this reaction. Full article
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Graphical abstract
Full article ">Figure 1
<p>Aza-Michael addition of imide (<b>1</b>) to fumaric esters.</p> Full article ">
441 KiB  
Review
Plant Phenolics: Extraction, Analysis and Their Antioxidant and Anticancer Properties
by Jin Dai and Russell J. Mumper
Molecules 2010, 15(10), 7313-7352; https://doi.org/10.3390/molecules15107313 - 21 Oct 2010
Cited by 3042 | Viewed by 88805
Abstract
Phenolics are broadly distributed in the plant kingdom and are the most abundant secondary metabolites of plants. Plant polyphenols have drawn increasing attention due to their potent antioxidant properties and their marked effects in the prevention of various oxidative stress associated diseases such [...] Read more.
Phenolics are broadly distributed in the plant kingdom and are the most abundant secondary metabolites of plants. Plant polyphenols have drawn increasing attention due to their potent antioxidant properties and their marked effects in the prevention of various oxidative stress associated diseases such as cancer. In the last few years, the identification and development of phenolic compounds or extracts from different plants has become a major area of health- and medical-related research. This review provides an updated and comprehensive overview on phenolic extraction, purification, analysis and quantification as well as their antioxidant properties. Furthermore, the anticancer effects of phenolics in-vitro and in-vivo animal models are viewed, including recent human intervention studies. Finally, possible mechanisms of action involving antioxidant and pro-oxidant activity as well as interference with cellular functions are discussed. Full article
(This article belongs to the Special Issue Antioxidants)
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<p>Structures of flavonoids, phenolic acids and tannins.</p> Full article ">Figure 2
<p>Structures of stilbenes and lignan.</p> Full article ">Figure 3
<p>Strategies for preparation and characterization of phenolic samples from plant materials. Abbreviations: MAE, microwave-assisted extraction; UAE, ultrasound-assisted extraction; PFE, pressurized fluid extraction; PLE, pressurized liquid extraction; ASE, accelerated solvent extraction; SWE, subcritical water extraction; SFE, supercritical fluid extraction; SPE, solid phase extraction; CCC, countercurrent chromatography; FD, Folin-Denis method (FD), F-C, Folin-Ciocalteu method; GC, gas chromatography; LC, Liquid chromatography; FLU, fluorescence; PDA, photodiode array; EAD, electro-array detection; ECD, electrochemical detection; MS, mass spectrometric; NMR, nuclear magnetic resonance.</p> Full article ">Figure 4
<p>Potential anticancer mechanisms of plant phenolics during cancer development.</p> Full article ">
686 KiB  
Article
Antioxidant-Prooxidant Properties of a New Organoselenium Compound Library
by Daniel Plano, Ylenia Baquedano, Elena Ibáñez, Iosu Jiménez, Juan Antonio Palop, Julian E. Spallholz and Carmen Sanmartín
Molecules 2010, 15(10), 7292-7312; https://doi.org/10.3390/molecules15107292 - 21 Oct 2010
Cited by 87 | Viewed by 13475
Abstract
The present study describes the biological evaluation of a library of 59 organo-selenium compounds as superoxide (O2) generators and cytotoxic agents in human prostate cancer cells (PC-3) and in breast adenocarcinoma (MCF-7). In order to corroborate that the biological activity [...] Read more.
The present study describes the biological evaluation of a library of 59 organo-selenium compounds as superoxide (O2) generators and cytotoxic agents in human prostate cancer cells (PC-3) and in breast adenocarcinoma (MCF-7). In order to corroborate that the biological activity for selenium compounds depends on the chemical form, a broad structural variety is presented. These structures include selenocyanates, diselenides, selenoalkyl functional moieties and eight newly synthesized symmetrically substituted dithioselenites and selenylureas. Eleven of the derivatives tested showed high levels of superoxide generation in vitro via oxidation of reduced glutathione (GSH) and nine of them were more catalytic than the reference compound, diselenodipropionic acid. Eighteen of the library compounds inhibited cell growth more than or similar to reference chemotherapeutic drugs in PC-3 and eleven were more potent cytotoxic agents than etoposide in the MCF-7 cell line. Considering both parameters (superoxide generation and cell cytotoxicity) compounds B1, C6 and C9 displayed the best therapeutic profiles. Considering that many diselenide compounds can generate superoxide (O2) in vitro via oxidation of GSH and other thiols, the analogue B1, that contains a diselenide moiety, was selected for a preliminary mechanistic investigation, which . revealed that B1 has apoptogenic effects similar to camptothecin mediated by reactive oxygen species (ROS) in lymphocytic leukemia cells (CCRF-CEM) and affected the MCF-7 cell-cycle in G2/M and S-phases. Full article
(This article belongs to the Special Issue Antioxidants)
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Figure 1
<p>A multi-tiered model of Se anticarcinogenesis.</p> Full article ">Figure 2
<p>Redox cycling of methylselenide and other selenides (RSe<sup>−</sup>).</p> Full article ">Figure 3
<p>Chemical structures of some representative selenium compounds with antioxidant properties.</p> Full article ">Figure 4
<p>General chemical structures for the series of compounds studied <b>A</b>-<b>D</b>.</p> Full article ">Figure 5
<p>Apoptotic effects of compound <b>B1</b> and camptothecin at 10 or 25 μM on CCRF-CEM and MCF-7 cells for 24 and 48 h, respectively. (<b>A</b>) Apoptotic effects of compound <b>B1</b> on CCRF-CEM were assessed by Flow Cytometry analysis after staining with Annexin V-FITC. Annexin V staining is represented on the x-axis and PI staining is represented on the y-axis. The representative results of three independent experiments are shown; (<b>B</b>) Apoptotic effects of compound <b>B1</b> were assessed by Flow Cytometry analysis using the <span class="html-italic">Apo-Direct</span> kit, based on the TUNEL assay; (<b>C</b>) Percentage of apoptotic and or necrotic cells after compound <b>B1</b> or camptothecin treatment were calculated from the flow cytometry results. Each bar represents the mean of three independent experiments and the error bars indicate standard deviation. ** p &lt; 0.01 with respect to the control.</p> Full article ">Figure 6
<p>Cell cycle profile of MCF-7 cells after 48 h treatment with compound <b>B1</b> and camptothecin at 25 μM. Each bar represents the mean of three independent experiments and error bars indicate the standard deviation. ** p &lt; 0.01 with respect to the control.</p> Full article ">Figure 7
<p>Intracellular content of ROS in CCRF-CEM cells after 4 and 24 h treatment with compound <b>B1</b> at 25 μM. (<b>A</b>) Flow Cytometry analysis is shown for 4 h treatment with compound <b>B1</b> or vehicle (control) for the representative results of three independent experiments; (<b>B</b>) Flow Cytometry analysis is shown for 24 h treatment with compound <b>B1</b> or vehicle (control) for the representative results of three independent experiments; (<b>C</b>) Each bar represents the mean of three independent experiments and the error bars indicate the standard deviation. ** p &lt; 0.01 with respect to the control.</p> Full article ">Scheme 1
<p>Synthetic routes for compounds related to dithioselenites and selenylureas (series <b>D</b>).</p> Full article ">
1002 KiB  
Review
The Nrf2 System as a Potential Target for the Development of Indirect Antioxidants
by Kyeong-Ah Jung and Mi-Kyoung Kwak
Molecules 2010, 15(10), 7266-7291; https://doi.org/10.3390/molecules15107266 - 20 Oct 2010
Cited by 387 | Viewed by 23672
Abstract
Oxidative stress causes damage to multiple cellular components such as DNA, proteins, and lipids, and is implicated in various human diseases including cancer, neurodegeneration, inflammatory diseases, and aging. In response to oxidative attack, cells have developed an antioxidant defense system to maintain cellular [...] Read more.
Oxidative stress causes damage to multiple cellular components such as DNA, proteins, and lipids, and is implicated in various human diseases including cancer, neurodegeneration, inflammatory diseases, and aging. In response to oxidative attack, cells have developed an antioxidant defense system to maintain cellular redox homeostasis and to protect cells from damage. The thiol-containing small molecules (e.g. glutathione), reactive oxygen species-inactivating enzymes (e.g. glutathione peroxidase), and phase 2 detoxifying enzymes (e.g. NAD(P)H: quinine oxidoreductase 1 and glutathione-S-transferases) are members of this antioxidant system. NF-E2-related factor 2 (Nrf2) is a CNC-bZIP transcription factor which regulates the basal and inducible expression of a wide array of antioxidant genes. Following dissociation from the cytosolic protein Keap1, a scaffolding protein which binds Nrf2 and Cul3 ubiquitin ligase for proteasome degradation, Nrf2 rapidly accumulates in the nucleus and transactivates the antioxidant response element in the promoter region of many antioxidant genes. The critical role of Nrf2 has been demonstrated by various animal studies showing that mice with a targeted disruption of the nrf2 gene are prone to develop lesions in response to environmental toxicants/carcinogens, drugs, and inflammatory insults. In this review, we discuss the role of the Nrf2 system, with particular focus on Nrf2-controlled target genes and the potential pleiotropic effects of Nrf2 activation of indirect antioxidants. Full article
(This article belongs to the Special Issue Antioxidants)
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Figure 1
<p>Nrf2 and its regulation by Keap1. (A) Under normal conditions, Nrf2 is degraded by Keap1-Cul3-dependent pathway; (B) In the presence of indirect antioxidants, Keap1-Nrf2 binding is disturbed and Nrf2 transactivates ARE-driven genes in the nucleus; (C) Protein structure of Keap1 and reactive cysteine residues for the action of Nrf2.</p> Full article ">
1029 KiB  
Review
Protecting Groups in Carbohydrate Chemistry: Influence on Stereoselectivity of Glycosylations
by Jian Guo and Xin-Shan Ye
Molecules 2010, 15(10), 7235-7265; https://doi.org/10.3390/molecules15107235 - 20 Oct 2010
Cited by 143 | Viewed by 21128
Abstract
Saccharides are polyhydroxy compounds, and their synthesis requires complex protecting group manipulations. Protecting groups are usually used to temporarily mask a functional group which may interfere with a certain reaction, but protecting groups in carbohydrate chemistry do more than protecting groups usually do. [...] Read more.
Saccharides are polyhydroxy compounds, and their synthesis requires complex protecting group manipulations. Protecting groups are usually used to temporarily mask a functional group which may interfere with a certain reaction, but protecting groups in carbohydrate chemistry do more than protecting groups usually do. Particularly, protecting groups can participate in reactions directly or indirectly, thus affecting the stereochemical outcomes, which is important for synthesis of oligosaccharides. Herein we present an overview of recent advances in protecting groups influencing stereoselectivity in glycosylation reactions, including participating protecting groups, and conformation-constraining protecting groups in general. Full article
(This article belongs to the Special Issue Protecting Group in Organic Synthesis)
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Figure 30

Figure 30
<p>Branched oligosaccharides <b>7</b><b>5</b> and <b>7</b><b>6</b>.</p> Full article ">Figure 31
<p>Dioxocarbenium ion intermediates by remote participation.</p> Full article ">Figure 32
<p>Proposed mechanism for 4,6-<span class="html-italic">O</span>-benzylidene-directed β-mannosylation.</p> Full article ">Figure 33
<p><span class="html-italic">N</span>-Acetyl 2,3-<span class="html-italic">trans</span>-oxazolidinone-protected donors <b>1</b><b>48-1</b><b>51</b>.</p> Full article ">Figure 34
<p>Plausible reaction mechanism of the donor <b>159</b>.</p> Full article ">Figure 35
<p>Proposed reaction mechanism for the DTBS-directed α-galactosylation.</p> Full article ">Figure 36
<p>A fragment of arabinogalactans in the primary plant cell wall.</p> Full article ">Figure 37
<p>The influence of the 3,4-O-bisacetal group onglycosylation selectivity.</p> Full article ">Scheme 1
<p>The stereoselective formation of glycosidic bond by neighboring-group participation.</p> Full article ">Scheme 2
<p>The formation of 1,2-trans glycosides directed by improved ester groups.</p> Full article ">Scheme 3
<p>Dialkyl phosphates as stereodirecting groups.</p> Full article ">Scheme 4
<p>Plausible mechanism of alkyl phosphates as 1,2-<span class="html-italic">trans</span> stereodirecting groups.</p> Full article ">Scheme 5
<p>Arming participating group for stereoselective glycosylation: <b>a)</b> synthesis of a trans, trans-linked trisaccharide <b>32</b>; <b>b)</b> proposed reaction mechanism.</p> Full article ">Scheme 6
<p>The mechanism of chiral auxiliary group participating.</p> Full article ">Scheme 7
<p>Preparation of donors having auxiliary ethyl mandelate.</p> Full article ">Scheme 8
<p>Stereoselective glycosylations with glycosyl donors <b>50</b> and <b>55</b>.</p> Full article ">Scheme 9
<p>Preparation of donors having auxiliary (<span class="html-italic">S</span>)-(phenylthiomethyl)benzyl group.</p> Full article ">Scheme 10
<p>Stereoselective glycosylations with glycosyl donors <b>59</b> and <b>62</b>.</p> Full article ">Scheme 11
<p>The mechanism of (<span class="html-italic">S</span>)-(phenylthiomethyl)benzyl moiety participation.</p> Full article ">Scheme 12
<p>One-pot two-step synthesis of trisaccharide <b>7</b><b>4</b>.</p> Full article ">Scheme 13
<p>Synthesis of a heptasaccharide from Gram-negative bacterium.</p> Full article ">Scheme 14
<p>Synthesis of 2-deoxyglycosides using donors with different protecting groups at O6 position.</p> Full article ">Scheme 15
<p>Comparison of influence of different groups at C3 on stereoselectivity.</p> Full article ">Scheme 16
<p>Comparison of influence of different groups at C3 on stereoselectivityin the synthesis of 3-amino-3-deoxy-mannopyranosides.</p> Full article ">Scheme 17
<p>Remote participation by non-vicinal esters.</p> Full article ">Scheme 18
<p>The comparison of α-directing effect with <span class="html-italic">O</span>-acyl group at different positions in mannopyranosylations and trapping of the intermediate.</p> Full article ">Scheme 19
<p>β-Mannosylation reactions with 4,6-<span class="html-italic">O</span>-benzylidenated mannosyl donors.</p> Full article ">Scheme 20
<p>β-Rhamnosides prepared from 4,6-<span class="html-italic">O</span>-benzylidenated mannosyl donors.</p> Full article ">Scheme 21
<p>Glycosylation reactionsof carbonate-protected donors.</p> Full article ">Scheme 22
<p>The preparation and glycosylation reactions of oxazolidinone-protecting donors.</p> Full article ">Scheme 23
<p>α-Sialylation using the oxazolidinone-protected donor.</p> Full article ">Scheme 24
<p>The silylene and oxazolidinone double-locked donors and α-sialylation with them.</p> Full article ">Scheme 25
<p>The glycosylation reaction with the donor having di-<span class="html-italic">tert-</span>butylsilylene.</p> Full article ">Scheme 26
<p>The β-selective furanosylation with 3,5-<span class="html-italic">O</span>-di-<span class="html-italic">tert-</span>butylsilylene-protected arabinosyl donor <b>178</b>.</p> Full article ">Scheme 27
<p>The β-selective furanosylation with 3,5-<span class="html-italic">O</span>-tetraisopropyldisiloxanylidene-protected donor.</p> Full article ">Scheme 28
<p>Comparision of donors <b>187</b> and <b>189</b> in glycosylation.</p> Full article ">Scheme 29
<p>β-Arabinofuranosylation of 2,3-<span class="html-italic">O</span>-xylylene-protected arabinofuranosyl donor <b>194</b>.</p> Full article ">
174 KiB  
Communication
Efficient Microwave-Assisted Synthesis of 5-Deazaflavine Derivatives
by Jorge Trilleras, Luis Gabriel López, Dency José Pacheco, Jairo Quiroga, Manuel Nogueras, José M. de la Torre and Justo Cobo
Molecules 2010, 15(10), 7227-7234; https://doi.org/10.3390/molecules15107227 - 20 Oct 2010
Cited by 8 | Viewed by 8767
Abstract
A series of pyrimido[4,5-b]quinolines (5-deazaflavines), were synthesized by microwave assisted intramolecular cyclization. The N4-substituted-2,4-diamino-6-chloro-pyrimidine-5-carbaldehydes, were prepared by selective monoamination of 2-amino-4,6-dichloropyrimidine-5-carbaldehyde with aliphatic and aromatic amines. Full article
(This article belongs to the Section Organic Chemistry)
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Full article ">Figure 1
<p>5-deazaflavine (pyrimido[4,5-<span class="html-italic">b</span>]quinoline) ring system <b>I</b> and pyrimido[4,5-<span class="html-italic">b</span>]quinoxaline ring system <b>II</b>.</p> Full article ">Figure 2
<p>Pyrimido[4,5-<span class="html-italic">b</span>]quinoline derivatives synthesized.</p> Full article ">Figure 3
<p>Synthesis of pyrimido[4,5-<span class="html-italic">b</span>]quinolines derivatives <b>2-4</b>.</p> Full article ">Figure 4
<p>Acid-catalysed Bradsher-type cyclodehydration of diaryl aldehydes <b>1</b>.</p> Full article ">
222 KiB  
Article
Anthraquinones with Antiplasmodial Activity from the Roots of Rennellia elliptica Korth. (Rubiaceae)
by Che Puteh Osman, Nor Hadiani Ismail, Rohaya Ahmad, Norizan Ahmat, Khalijah Awang and Faridahanim Mohd Jaafar
Molecules 2010, 15(10), 7218-7226; https://doi.org/10.3390/molecules15107218 - 20 Oct 2010
Cited by 49 | Viewed by 10681
Abstract
Dichloromethane root extract of Rennellia elliptica Korth. showed strong inhibition of Plasmodium falciparum growth in vitro with an IC50 value of 4.04 µg/mL. A phytochemical study of the dichloromethane root extract has led to the isolation and characterization of a new anthraquinone, [...] Read more.
Dichloromethane root extract of Rennellia elliptica Korth. showed strong inhibition of Plasmodium falciparum growth in vitro with an IC50 value of 4.04 µg/mL. A phytochemical study of the dichloromethane root extract has led to the isolation and characterization of a new anthraquinone, 1,2-dimethoxy-6-methyl-9,10-anthraquinone (1), and ten known anthraquinones: 1-hydroxy-2-methoxy-6-methyl-9,10-anthraquinone (2), nordamnacanthal (3), 2-formyl-3-hydroxy-9,10-anthraquinone (4), damnacanthal (5), lucidin-ω-methyl ether (6), 3-hydroxy-2-methyl-9,10-anthraquinone (7), rubiadin (8), 3-hydroxy-2-methoxy-6-methyl-9,10-anthraquinone (9), rubiadin-1-methyl ether (10) and 3-hydroxy-2-hydroxymethyl-9,10-anthraquinone (11). Structural elucidation of all compounds was accomplished by modern spectroscopic methods, notably 1D and 2D NMR, IR, UV and HREIMS. The new anthraquinone 1, 2-formyl-3-hydroxy-9,10-anthraquinone (4) and 3-hydroxy-2-methyl-9,10-anthraquinone (7) possess strong antiplasmodial activity, with IC50 values of 1.10, 0.63 and 0.34 µM, respectively. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>Anthraquinones <b>1-11</b>, isolated from roots of <span class="html-italic">R. elliptica</span> Korth.</p> Full article ">Figure 2
<p>NOESY Correlations of <b>1</b>.</p> Full article ">
318 KiB  
Article
The Beneficial Effect of Vanillic Acid on Ulcerative Colitis
by Su-Jin Kim, Min-Cheol Kim, Jae-Young Um and Seung-Heon Hong
Molecules 2010, 15(10), 7208-7217; https://doi.org/10.3390/molecules15107208 - 19 Oct 2010
Cited by 135 | Viewed by 12679
Abstract
Vanillic acid, an oxidized form of vanillin, is a benzoic acid derivative used as a flavoring agent. The objective of this study was to determine whether vanillic acid has beneficial effects against dextran sulfate sodium (DSS)-induced ulcerative colitis. Our results showed that vanillic [...] Read more.
Vanillic acid, an oxidized form of vanillin, is a benzoic acid derivative used as a flavoring agent. The objective of this study was to determine whether vanillic acid has beneficial effects against dextran sulfate sodium (DSS)-induced ulcerative colitis. Our results showed that vanillic acid reduced the severity of the clinical signs of DSS-induced colitis, including weight loss and shortening of colon length, and the disease activity index. The results of this study showed that vanillic acid significantly suppressed the expression of cyclooxygenase-2 and the activation of transcription nuclear factor-kB p65 in DSS-treated colon tissues. In addition, we observed that the plasma levels of interleukin (IL)-6 were higher in the DSS-treated group than in the control group, but these increased levels were reduced by the administration of vanillic acid. Taken together, these findings suggest that vanillic acid has a beneficial effect on DSS-induced ulcerative colitis, thereby indicating its usefulness in the regulation of chronic intestinal inflammation. Full article
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Figure 1
<p>Effect of vanillic acid on the clinical signs in DSS-induced colitis. Experimental colitis in mice was induced by 7-day treatment with 5% DSS dissolved in drinking water. Vanillic acid was administered orally at doses of 200 mg/kg once a day for seven days before DSS treatment. (A) Body weight of the mice was measured. (B) The colons were removed on day 7 after DSS treatment, and the colon lengths were measured. (C) DAI was calculated. Mice treated with sulfasalazine (150 mg/kg) were used as positive controls. Data are represented as the mean (SEM) (n = 5) from triplicate experiments (<sup>#</sup> <span class="html-italic">P</span> &lt; 0.05 <span class="html-italic">vs.</span> control, * <span class="html-italic">P</span> &lt; 0.05 <span class="html-italic">vs.</span> DSS alone).</p> Full article ">Figure 2
<p>Effect of vanillic acid on the level of IL-6 in the plasma of DSS-treated mice. Experimental colitis in mice was induced by 7-day treatment with 5% DSS dissolved in the drinking water. Vanillic acid was administered orally at doses of 200 mg/kg once a day for seven days before DSS treatment. Mice treated with sulfasalazine (150 mg/kg) were used as positive controls. At the end of the experiment, blood samples were collected from all the mice and immediately centrifuged at 3,000 rpm for 15 min to separate the plasma. The levels of IL-6 in mouse plasma were evaluated by ELISA.</p> Full article ">Figure 3
<p>Effect of vanillic acid on the levels of COX-2 and NF-κB p65 in DSS-treated colon tissue. Experimental colitis was induced in mice by 7-day treatment with 5% DSS dissolved in drinking water. Vanillic acid was administered orally at doses of 200 mg/kg once a day for 7 days before DSS treatment. Mice treated with sulfasalazine (150 mg/kg) were used as positive controls. At the end of the experiment, the colon tissue was excised and homogenized. (A) The levels of COX-2 were evaluated by Western blot analysis. (B) The levels of NF-κB p65 were evaluated by Western blot analysis.</p> Full article ">
682 KiB  
Article
Small Interfering RNA Effectively Inhibits the Expression of SARS Coronavirus Membrane Gene at Two Novel Targeting Sites
by Ying Wang, Ying-Li Cao, Fan Yang, Yun Zhang, Shu-Hui Wang and Li Liu
Molecules 2010, 15(10), 7197-7207; https://doi.org/10.3390/molecules15107197 - 18 Oct 2010
Cited by 18 | Viewed by 10409
Abstract
Small interfering RNA (siRNA) is a class of duplex RNA molecules of 21-25 nt nucleotides in length functioning post-transcriptionally to downregulate targeted gene expression. The membrane (M) protein of severe acute respiratory syndrome-associated coronavirus (SARS-CoV) is highly abundant during viral infections and is [...] Read more.
Small interfering RNA (siRNA) is a class of duplex RNA molecules of 21-25 nt nucleotides in length functioning post-transcriptionally to downregulate targeted gene expression. The membrane (M) protein of severe acute respiratory syndrome-associated coronavirus (SARS-CoV) is highly abundant during viral infections and is a critical element for viral assembly. Nucleotide substitution in the viral genome occurs frequently during SARS-CoV infection. In the current study, we analyzed the M gene sequences derived from 15 SARS-CoV isolates and uncovered six nucleotide substitutions among these isolates. Interestingly, these nucleotide substitutions are all located at the 5’ half of the M gene. Based on this information and previous reports, we created two novel siRNAs targeting two unexploited and well conserved regions in the M gene. The effects of these two siRNAs were tested by semi-quantitative RT-PCR and EGFP-M fusion gene expression. The results demonstrated that both siRNAs effectively and specifically blocked the targeted gene expression. Real time quantitative RT-PCR (qRT-PCR) revealed that siRNA targeting the 3’ half of the M gene (si-M2) induced more potent inhibition than that targeting the 5’ half (si-M1). Both si-M1 and si-M2 significantly downregulated M gene mediated upregulation of interferon b expression. Thus, our results indicate that SARS-CoV M gene specific siRNA might function in a sequence-dependent manner. Full article
(This article belongs to the Special Issue Catalytic Nucleic Acids)
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<p>Sequence alignment of the M genes of different SARS-CoV isolates. Two novel siRNAs (si-M1 and si-M2) targeting at 221~242nt and 466~486nt, respectively, are underlined.</p> Full article ">Figure 2
<p>Cloning and expression analysis of SARS-CoV M gene. (a) M gene was cloned by RT-PCR. (b) Western blot analysis on M gene expression in HEK293T cells. HEK293T cells were transfected with either pCMV-Myc or pCMV-Myc-M. After 48 h, the transfected cells were lysed and subjected to brief centrifugation to separate supernatant from cell pellet. Equal amount of cell supernatant and pellet were resolved onto 12% SDS-PAGE. The reaction products were probed with anti-Myc antibody.</p> Full article ">Figure 3
<p>The inhibitory effect of siRNA1 on SARS-CoV M gene expression. (a)RT-PCR analysis on si-M1 mediated M gene repression. About 1μg of pCMV-Myc-M was co-transfected with increased doses of si-M1. The reaction products were subjected to RT-PCR analysis using SARS-M and GAPDH primers. (b) Quantitation of the RT-PCR results in (a). (c) si-M1 specifically inhibited pEGFP-M fusion gene but not pEGFP gene expression. About 1μg of either pEGFP-M or pEGFP was co-transfected with increased doses of si-M1. (d) si-M1 but not si-IL-17RE effectively inhibited EGFP-M gene expression. About 1μg of pEGFP-M plasmid was co-transfected with increased doses of either si-M1 or si-IL17RE. (e) Flow cytometric analysis on the intensity of pEGFP-M gene expression in (d).</p> Full article ">Figure 4
<p>The inhibitory effect of siRNA2 on SARS-CoV M gene expression. (a) RT-PCR analysis on the dose effect of si-M2 on M mRNA expression. About 1 μg of pCMV-Myc-M was co-transfected with increased doses of si-M2. The reaction products were subjected to RT-PCR analysis using SARS-M and GAPDH primers. (b) Quantitation of the RT-PCR results in (a). (c) si-M2 specifically inhibited pEGFP-M fusion gene but not pEGFP gene expression. About 1 μg of either pEGFP-M or pEGFP was co-transfected with increased doses of si-M2. (d) si-M2 but not si-IL-17RE effectively inhibited pEGFP-M gene expression. About 1 μg of pEGFP-M plasmid was co-transfected with increased doses of either si-M2 or si-IL17RE. (e) Flow cytometric analysis on the intensity of pEGFP-M gene expression in (d).</p> Full article ">Figure 5
<p>Comparison of the inhibitory effect mediated by si-M1, si-M2 and si-M3 on M gene expression by qRT-PCR analysis. About 2 μg of M gene was co-transfected with 4 μg of each plasmid pBS/U6, si-M1, si-M2 and si-M3, while co-transfection of 2 μg of pCMV-Myc plus 4 μg of pBS/U6 was served as negative control. Both β-actin-R and SARS-M-R primers were used in this analysis.</p> Full article ">Figure 6
<p>The counteractive effect of si-M1 and siM2 on M gene mediated interferon β production. HEK293 cells were co-transfected with 2 μg plasmid pCMV-Myc-M plus 4 μg of each pBS/U6 (lane 2), pBS/U6-siM1 (lane 3) or pBS/U6-siM2 (lane 4). Co-transfection of 2 μg pCMV-Myc plus 4 μg of pBS/U6 was served as negative control (lane 1). About 1 μg of total RNA isolated from each reaction was subjected to RT-PCR analysis using either IFNβ or β-actin primers.</p> Full article ">
222 KiB  
Article
Preparation of a Carbon-Based Solid Acid Catalyst by Sulfonating Activated Carbon in a Chemical Reduction Process
by Xiao-Yan Liu, Miao Huang, Hai-Long Ma, Zeng-Qiang Zhang, Jin-Ming Gao, Yu-Lei Zhu, Xiao-Jin Han and Xiang-Yun Guo
Molecules 2010, 15(10), 7188-7196; https://doi.org/10.3390/molecules15107188 - 18 Oct 2010
Cited by 306 | Viewed by 19718
Abstract
Sulfonated (SO3H-bearing) activated carbon (AC-SO3H) was synthesized by an aryl diazonium salt reduction process. The obtained material had a SO3H density of 0.64 mmol·g-1 and a specific surface area of 602 m2·g-1. [...] Read more.
Sulfonated (SO3H-bearing) activated carbon (AC-SO3H) was synthesized by an aryl diazonium salt reduction process. The obtained material had a SO3H density of 0.64 mmol·g-1 and a specific surface area of 602 m2·g-1. The catalytic properties of AC-SO3H were compared with that of two commercial solid acid catalysts, Nafion NR50 and Amberlyst-15. In a 10-h esterification reaction of acetic acid with ethanol, the acid conversion with AC-SO3H (78%) was lower than that of Amberlyst-15 (86%), which could be attributed to the fact that the SO3H density of the sulfonated carbon was lower than that of Amberlyst-15 (4.60 mmol·g-1). However, AC-SO3H exhibited comparable and even much higher catalytic activities than the commercial catalysts in the esterification of aliphatic acids with longer carbon chains such as hexanoic acid and decanoic acid, which may be due to the large specific surface area and mesoporous structures of the activated carbon. The disadvantage of AC-SO3H is the leaching of SO3H group during the reactions. Full article
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<p>XRD patterns for activated carbon (a) before and (b) after sulfonation.</p> Full article ">Figure 2
<p>S 2p XPS spectrum of AC-SO<sub>3</sub>H.</p> Full article ">Figure 3
<p>Thermogravimetric profiles for (a) AC, (b) AC-SO<sub>3</sub>H.</p> Full article ">Figure 4
<p>N<sub>2</sub> adsorption isotherms of (a) AC and (b) AC-SO<sub>3</sub>H.</p> Full article ">Figure 5
<p>Acid catalyzed esterification of several aliphatic acids with ethanol: (a) acetic acid, (b) hexanoic acid, and (c) decanoic acid.</p> Full article ">Figure 6
<p>Variation of the SO<sub>3</sub>H density on the carbon catalysts in a series of 2-h acetic acid esterification reaction cycles.</p> Full article ">
173 KiB  
Review
Role of Oxidant Scavengers in the Prevention of Ca2+ Homeostasis Disorders
by Carmen Galan, Isaac Jardín, Natalia Dionisio, Ginés Salido and Juan A. Rosado
Molecules 2010, 15(10), 7167-7187; https://doi.org/10.3390/molecules15107167 - 15 Oct 2010
Cited by 19 | Viewed by 10550
Abstract
A number of disorders, such as Alzheimer disease and diabetes mellitus, have in common the alteration of the redox balance, resulting in an increase in reactive oxygen species (ROS) generation that might lead to the development of apoptosis and cell death. It has [...] Read more.
A number of disorders, such as Alzheimer disease and diabetes mellitus, have in common the alteration of the redox balance, resulting in an increase in reactive oxygen species (ROS) generation that might lead to the development of apoptosis and cell death. It has long been known that ROS can significantly alter Ca2+ mobilization, an intracellular signal that is involved in the regulation of a wide variety of cellular functions. Cells have a limited capability to counteract the effects of oxidative stress, but evidence has been provided supporting the beneficial effects of exogenous ROS scavengers. Here, we review the effects of oxidative stress on intracellular Ca2+ homeostasis and the role of antioxidants in the prevention and treatment of disorders associated to abnormal Ca2+ mobilization induced by ROS. Full article
(This article belongs to the Special Issue Antioxidants)
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443 KiB  
Article
Mechanisms of the Gastric Antiulcerogenic Activity of Anacardium humile St. Hil on Ethanol-Induced Acute Gastric Mucosal Injury in Rats
by Anderson Luiz-Ferreira, Ana Cristina Alves de Almeida, Maíra Cola, Victor Barbastefano, Ana Beatriz Albino de Almeida, Leônia Maria Batista, Elisângela Farias-Silva, Cláudia Helena Pellizzon, Clélia Akiko Hiruma-Lima, Lourdes Campaner Santos, Wagner Vilegas and Alba Regina Monteiro Souza Brito
Molecules 2010, 15(10), 7153-7166; https://doi.org/10.3390/molecules15107153 - 15 Oct 2010
Cited by 37 | Viewed by 14654
Abstract
Leaves and bark infusions Anacardium humile St. Hil. (Anacardiaceae), known as in Brazil as “cajuzinho do cerrado”, have been used in folk medicine as an alternative treatment for ulcers and gastritis. This study evaluated the gastroprotective activity of an ethyl acetate extract of [...] Read more.
Leaves and bark infusions Anacardium humile St. Hil. (Anacardiaceae), known as in Brazil as “cajuzinho do cerrado”, have been used in folk medicine as an alternative treatment for ulcers and gastritis. This study evaluated the gastroprotective activity of an ethyl acetate extract of the leaves of A. humile (AcF) and the mechanism involved in this gastroprotection. Pretreatment concentrations (50, 100, 200 mg.kg−1) were administered by gavage. Following a 60 min. period, all the rats were orally administered 1 mL of absolute ethanol. One hour after the administration of ethanol, all groups were sacrificed, and the gastric ulcer index was calculated. Prostaglandin PGE2 concentration, gastric adherent mucous, and the participation of nitric oxide (NO) and sulfhydryl compounds in the gastroprotection process were also analyzed using the most effective tested dose (50 mg·kg−1). A histological study of the glandular stomach for the evaluation of the epithelial damage and mucus content was also performed. AcF significantly reduced the gastric damage produced by ethanol. This effect was statistically significant for the 50 mg·kg−1 group compared to control. Also, it significantly increased the PGE2 (by 10-fold) and mucous production, while pretreatment with NG-nitro-L-arginine methyl ester (L-NAME) or N-ethylmaleimide (NEM) completely abolished the gastroprotection. AcF has a protective effect against ethanol, and this effect, might be due to the augmentation of the protective mechanisms of mucosa. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>Compounds found in the leaves of <span class="html-italic">Anacardium humile</span> St. Hil.</p> Full article ">Figure 2
<p><b>A.</b> HPLC chromatographic profile of the AcF from <span class="html-italic">A. humile</span> monitored at 210 nm. 1. Gallic acid, a. Unknown, b. Unkown catechin, 2. Methyl gallate, 3. (+)-catechin, c. Gallic acid derivative, 7. Amenthoflavone, * Flavonoid glycosides and gallic acid derivatives. <b>B.</b> Elution monitored at 360 nm for flavonol glycosides.</p> Full article ">Figure 3
<p>Photomicrography of stomach gastric ulceration caused by ethanol.</p> Full article ">Figure 4
<p>Effects of orally administered ethyl acetate extract (AcF; 50 mg·kg<sup>−1</sup>) obtained from the leaves of <span class="html-italic">A</span>. <span class="html-italic">Humile</span> St. Hil. and indomethacin on gastric prostaglandin E<sub>2</sub> (PGE<sub>2</sub>) production in rats.</p> Full article ">Figure 5
<p>Effects of orally administered ethyl acetate extract (AcF; 50 mg·kg<sup>−1</sup>) obtained from the leaves of <span class="html-italic">A. humile</span> St. Hil. and of carbenoxolone (200 mg·kg<sup>−1</sup>) on adherent gastric mucous (measured as the amount of alcian blue bound) in pylorus-ligated rats.</p> Full article ">Figure 6
<p>Photomicrography of stomach showing the mucosal layer stained with PAS showing mucus in (A) normal epithelium; (B) loss of epithelial mucus in Tween treatment and (C) presence of epithelial mucus after AcF treatment.</p> Full article ">Figure 7
<p>Effects of orally administered ethyl acetate extract (AcF; 50 mg·kg<sup>−1</sup>) obtained from the leaves of <span class="html-italic">A. humile</span> St. Hil. and of carbenoxolone (100 mg·kg<sup>−1</sup>) on ethanol-induced gastric ulcers in rats pretreated with L-NAME.</p> Full article ">Figure 8
<p>Effects of orally administered ethyl acetate extract (AcF; 50 mg·kg<sup>−1</sup>) obtained from the leaves of <span class="html-italic">A. humile</span> St. Hil. and of carbenoxolone (100 mg·kg<sup>−1</sup>) on ethanol-induced gastric ulcers in rats pretreated with NEM.</p> Full article ">
233 KiB  
Article
Anti-Adhesive Activities of Flavan-3-ols and Proanthocyanidins in the Interaction of Group A-Streptococci and Human Epithelial Cells
by Aneta Janecki and Herbert Kolodziej
Molecules 2010, 15(10), 7139-7152; https://doi.org/10.3390/molecules15107139 - 15 Oct 2010
Cited by 32 | Viewed by 10980
Abstract
Bacterial adhesion to epithelial cells is a key step in infections, allowing subsequent colonization, invasion and internalization of pathogens into tissues. Anti-adhesive agents are therefore potential prophylactic tools against bacterial infections. The range of anti-adhesive compounds is largely confined to carbohydrate analogues. Tannins [...] Read more.
Bacterial adhesion to epithelial cells is a key step in infections, allowing subsequent colonization, invasion and internalization of pathogens into tissues. Anti-adhesive agents are therefore potential prophylactic tools against bacterial infections. The range of anti-adhesive compounds is largely confined to carbohydrate analogues. Tannins are generously recognized as potent antimicrobials, but little data exist on their anti-adherence potency. Using a model for mucosal pathogenesis with labeled group A-streptococci (GAS) and human laryngeal HEp-2 cells, a series of flavan-3-ols (epicatechin, epigallocatechin, epigallocatechin-3-O-gallate) and highly purified and chemically characterized proanthocyanidin samples including procyanidins based on epicatechin, catechin or ‘mixed’ constituent flavanyl units, prodelphinidins made up of (epi)gallocatechin monomeric unts as well as oligomers possessing A-type units in their molecules was evaluated for anti-adhesive effects. Reduced microbial adherence was observed exclusively for prodelphinidins, suggesting that pyrogallol-type elements, i.e., (epi)gallocatechin units are important structural features. This is the first report on structure-activity relationships regarding the anti-adhesive potency of proanthocyanidins. In addition, the structures of the first chemically defined proanthocyanidins from Pelargonium sidoides are disclosed. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>Flow cytometry-based anti-adhesive assay.</p> Full article ">Figure 2
<p>Structures of flavan-3-ols.</p> Full article ">Figure 3
<p>Adhesion of GAS pre-treated with the flavan-3-ols EC (<b>1</b>), EGC (<b>2</b>) and EGCG (<b>3</b>) to human HEp-2 cells as assessed by FACS analysis.Data represent the mean ± SD of epithelial cells that showed fluorescent bacteria and are derived from at least three independent experiments (* p &lt; 0.05; ** p&lt; 0.01; *** p&lt; 0.001).</p> Full article ">Figure 4
<p>Structures of oligomeric proanthocyanidins.</p> Full article ">Figure 5
<p>Adhesion of GAS pre-treated with purified A- and B-type procyanidin samples to human HEp-2 cells as assessed by FACS analysis. Data represent the mean ± SD of epithelial cells that showed fluorescent bacteria and are derived from at least three independent experiments (* p &lt; 0.05).</p> Full article ">Figure 6
<p>Effect of prodelphinidin samples on the adhesion of calcein-AM stained GAS to human HEp-2 cells as assessed by FACS analysis. Data represent the mean ± SD of epithelial cells that showed fluorescent bacteria and are derived from at least three independent experiments (* p &lt; 0.05; ** p &lt; 0.01; *** p &lt; 0.001).</p> Full article ">Figure 7
<p>Structures of proanthocyanidins <b>4</b>-<b>7</b>.</p> Full article ">
276 KiB  
Article
Effects of Different Maturity Stages on Antioxidant Content of Ivorian Gnagnan (Solanum indicum L.) Berries
by Denis N’Dri, Luca Calani, Teresa Mazzeo, Francesca Scazzina, Massimiliano Rinaldi, Daniele Del Rio, Nicoletta Pellegrini and Furio Brighenti
Molecules 2010, 15(10), 7125-7138; https://doi.org/10.3390/molecules15107125 - 15 Oct 2010
Cited by 34 | Viewed by 10701
Abstract
Gnagnan (Solanum indicum L.) is a spontaneous plant widely distributed in Ivory Coast. During ripening stages, Solanum indicum L. presents different colours (green, yellow and red) and is reported to contain several albeit poorly characterized antioxidant compounds. This paper describes in detail [...] Read more.
Gnagnan (Solanum indicum L.) is a spontaneous plant widely distributed in Ivory Coast. During ripening stages, Solanum indicum L. presents different colours (green, yellow and red) and is reported to contain several albeit poorly characterized antioxidant compounds. This paper describes in detail the antioxidant profile (ascorbic acid, carotenoids and polyphenols), antioxidant capacity (FRAP test and Folin-Ciocalteau assay) and the colour changes of Gnagnan berries at different ripening levels. Ascorbic acid content was similar in green and yellow berries, but significantly lower in red ones. Red berries showed a higher content of carotenoids compared to green and yellow ones. Regarding polyphenols, several phenolic acids and flavonoids were found in all berries. The content of caffeoylquinic acids, caffeic acid, flavonol glycosides and naringenin was higher in red berries, while the content of p-coumaric acid and feruloylquinic acids was similar among the three colours. The FRAP assay increased with the ripening process, whereas total polyphenols were similar among berries. Significant differences were found for the colorimetric indexes among products of different degrees of ripening. The present results show the important role of the ripening stage in increasing the antioxidant content of Gnagnan berries. Full article
(This article belongs to the Special Issue Antioxidants)
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Full article ">Figure 1
<p><span class="html-italic">Solanum indicum </span>L. berries at different ripening stages (green, A; yellow, B; red, C).</p> Full article ">Figure 2
<p>Chromatogram of carotenoids in red (<sup>___</sup>) and yellow (----) <span class="html-italic">Solanum indicum </span>L. berries. A: lycopene; B: α-carotene; C: β-carotene.</p> Full article ">Figure 3
<p>HPLC-ESI-MS/MS chromatograms of main flavonoids in red <span class="html-italic">Solanum indicum </span>L..</p> Full article ">Figure 4
<p>HPLC-ESI-MS/MS chromatograms of main phenolic acids in red <span class="html-italic">Solanum indicum </span>L..</p> Full article ">Figure 5
<p>Factor analysis biplots for Gnagnan maturity stage : (A) variables loadings; (B) score loadings.</p> Full article ">
232 KiB  
Article
Inhibitory Effects of Resveratrol on the Epstein-Barr Virus Lytic Cycle
by Ching-Yi Yiu, Shih-Ying Chen, Li-Kwan Chang, Ya-Fang Chiu and Tsuey-Pin Lin
Molecules 2010, 15(10), 7115-7124; https://doi.org/10.3390/molecules15107115 - 14 Oct 2010
Cited by 57 | Viewed by 11583
Abstract
Reactivation of Epstein-Barr virus (EBV) from latency to the lytic cycle is required for the production of viral particles. Here, we examine the capacity of resveratrol to inhibit the EBV lytic cycle. Our results show that resveratrol inhibits the transcription of EBV immediate [...] Read more.
Reactivation of Epstein-Barr virus (EBV) from latency to the lytic cycle is required for the production of viral particles. Here, we examine the capacity of resveratrol to inhibit the EBV lytic cycle. Our results show that resveratrol inhibits the transcription of EBV immediate early genes, the expression of EBV lytic proteins, including Rta, Zta, and EA-D and reduces viron production, suggesting that this compound may be useful for preventing the proliferation of the virus. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>Effect of resveratrol on cell viability.</p> Full article ">Figure 2
<p>Indriect immunofluorescence analysis of inhibition effects on the expression of EBV lytic genes.</p> Full article ">Figure 3
<p>Inhibition of the expression of EBV lytic proteins by resveratrol.</p> Full article ">Figure 4
<p>Inhibition of the transcription of the BRLF1 and BZLF1 promoters by resveratrol.</p> Full article ">Figure 5
<p>Resveratrol treatment and production of EBV particles.</p> Full article ">
205 KiB  
Article
A New Xanthone from the Bark Extract of Rheedia acuminata and Antiplasmodial Activity of Its Major Compounds
by Guillaume Marti, Véronique Eparvier, Marc Litaudon, Philippe Grellier and Françoise Guéritte
Molecules 2010, 15(10), 7106-7114; https://doi.org/10.3390/molecules15107106 - 14 Oct 2010
Cited by 18 | Viewed by 8309
Abstract
Bioassay-guided fractionation of the ethyl acetate bark extract of Rheedia acuminata led to the isolation of the new compound 1,5,6-trihydroxy-3-methoxy-7-geranyl-xanthone (1), together with four known compounds 2-5. These compounds were tested in vitro for their antiplasmodial activity on [...] Read more.
Bioassay-guided fractionation of the ethyl acetate bark extract of Rheedia acuminata led to the isolation of the new compound 1,5,6-trihydroxy-3-methoxy-7-geranyl-xanthone (1), together with four known compounds 2-5. These compounds were tested in vitro for their antiplasmodial activity on a chloroquine-resistant strain of Plasmodium falciparum (FcB1) and for their cytotoxicity against the human diploid embryonic lung cell line MRC-5. Full article
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<p>Structures of compounds <b>1</b>-<b>5</b>.</p> Full article ">Figure 2
<p>Key COSY (bold), HMBC (plain arrows) and NOESY (dashed arrows) correlations for <b>1</b>.</p> Full article ">
77 KiB  
Review
Bignoniaceae Metabolites as Semiochemicals
by Lucía Castillo and Carmen Rossini
Molecules 2010, 15(10), 7090-7105; https://doi.org/10.3390/molecules15107090 - 14 Oct 2010
Cited by 20 | Viewed by 9971
Abstract
Members of the family Bignoniaceae are mostly found in tropical and neo-tropical regions in America, Asia and Africa, although some of them are cultivated in other regions as ornamentals. Species belonging to this family have been extensively studied in regard to their pharmacological [...] Read more.
Members of the family Bignoniaceae are mostly found in tropical and neo-tropical regions in America, Asia and Africa, although some of them are cultivated in other regions as ornamentals. Species belonging to this family have been extensively studied in regard to their pharmacological properties (as extracts and isolated compounds). The aim of this review is to summarize the reported scientific evidence about the chemical properties as well as that of the extracts and isolated compounds from species of this family, focusing mainly in insect-plant interactions. As it is known, this family is recognized for the presence of iridoids which are markers of oviposition and feeding preference to species which have became specialist feeders. Some herbivore species have also evolved to the point of been able to sequester iridoids and use them as defenses against their predators. However, iridoids also exhibit anti-insect properties, and therefore they may be good lead molecules to develop botanical pesticides. Other secondary metabolites, such as quinones, and whole extracts have also shown potential as anti-insect agents. Full article
(This article belongs to the Special Issue Phytochemicals with Signaling, Medicinal and Therapeutic Properties)
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<p>Examples of Bignoniaciae iridiods.</p> Full article ">Figure 2
<p>Naphthoquinones and miscellaneous chemicals.</p> Full article ">
138 KiB  
Article
Two New Alkaloids from Narcissus serotinus L.
by Natalia B. Pigni, Strahil Berkov, Abdelaziz Elamrani, Mohammed Benaissa, Francesc Viladomat, Carles Codina and Jaume Bastida
Molecules 2010, 15(10), 7083-7089; https://doi.org/10.3390/molecules15107083 - 14 Oct 2010
Cited by 20 | Viewed by 10909
Abstract
The Amaryllidaceae family is well known for the presence of an exclusive group of alkaloids with a wide range of biological activities. Narcissus serotinus L. is a plant belonging to this family and its geographical distribution is mainly located along the Mediterranean coast. [...] Read more.
The Amaryllidaceae family is well known for the presence of an exclusive group of alkaloids with a wide range of biological activities. Narcissus serotinus L. is a plant belonging to this family and its geographical distribution is mainly located along the Mediterranean coast. In the present work, specimens collected near Casablanca (Morocco) were used to study the alkaloid content of this species. Starting with 350 g of the whole plant we used standard extraction and purification procedures to obtain fractions and compounds for GC-MS and NMR analysis. As well as five known alkaloids, we isolated two new compounds: 1-O-(3´-acetoxybutanoyl)lycorine and narseronine. The latter has been previously published, but with an erroneous structure. Full article
(This article belongs to the Section Natural Products Chemistry)
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<p>New alkaloids isolated from <span class="html-italic">N. serotinus</span> L. 1-<span class="html-italic">O</span>-(3´-acetoxybutanoyl)lycorine (<b>1</b>) and narseronine (<b>2</b>).</p> Full article ">
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