439 research outputs found

    Optical properties of substituted phthalocyanine rare-earth metal complexes

    Get PDF
    Comparative study of optical properties of alkylthio-group-substituted phthalocyanine rare-earth metal sandwich complexes ([(CnS)(8)Pc](2)M,M=Eu,Lu,Tb) is presented. Photoluminescence and photoconductivity of [(CnS)(8)Pc](2)M complex is very weak. Two photoluminescence bands were observed at around 400-650 and 720-800 nm in chloroform solution corresponding to the Soret and Q bands in the absorption spectra, respectively. However, the emission from Eu3+ ion (as well as Tb3+) was not found compared with other Eu complexes because the 5d levels of the Eu3+ ion lie higher than the triplet level of the ligand. The significant enhancement of the photoconductivity of [(C16S)(8)Pc](2)M after C-60 doping is reported. The photoconductivity is positive at the low electric field in the ohmic regime while it becomes negative at the high electric field upon photoexcitation with strongly absorbed light. The negative photoconductivity is attributed to space-charge effects. The mechanism of photoluminescence and photoconductivity are discussed by taking the electronic energy schemes of phthalocyanine ligands and lanthanide ion and C-60 into consideration.ArticleJOURNAL OF APPLIED PHYSICS. 88(12):7137-7143 (2000)journal articl

    Points, Walls and Loops in Resonant Oscillatory Media

    Full text link
    In an experiment of oscillatory media, domains and walls are formed under the parametric resonance with a frequency double the natural one. In this bi-stable system, %phase jumps π\pi by crossing walls. a nonequilibrium transition from Ising wall to Bloch wall consistent with prediction is confirmed experimentally. The Bloch wall moves in the direction determined by its chirality with a constant speed. As a new type of moving structure in two-dimension, a traveling loop consisting of two walls and Neel points is observed.Comment: 9 pages (revtex format) and 6 figures (PostScript

    Optical properties of substituted phthalocyanine rare-earth metal complexes

    Full text link
    Comparative study of optical properties of alkylthio-group-substituted phthalocyanine rare-earth metal sandwich complexes ([(CnS)8Pc]2M,M=Eu,Lu,Tb) is presented. Photoluminescence and photoconductivity of [(CnS)8Pc]2M complex is very weak. Two photoluminescence bands were observed at around 400–650 and 720–800 nm in chloroform solution corresponding to the Soret and Q bands in the absorption spectra, respectively. However, the emission from Eu3+ ion (as well as Tb3+) was not found compared with other Eu complexes because the 5d levels of the Eu3+ ion lie higher than the triplet level of the ligand. The significant enhancement of the photoconductivity of [(C16S)8Pc]2M after C60 doping is reported. The photoconductivity is positive at the low electric field in the ohmic regime while it becomes negative at the high electric field upon photoexcitation with strongly absorbed light. The negative photoconductivity is attributed to space-charge effects. The mechanism of photoluminescence and photoconductivity are discussed by taking the electronic energy schemes of phthalocyanine ligands and lanthanide ion and C60 into consideration.This article may be downloaded for personal use only. Any other use requires prior permission of the author and AIP Publishing. This article appeared in K. Yoshino, S. B. Lee, T. Sonoda, H. Kawagishi, R. Hidayat, K. Nakayama, M. Ozaki, K. Ban, K. Nishizawa, K. Ohta, and H. Shirai, Journal of Applied Physics 88, 7137 (2000) and may be found at https://doi.org/10.1063/1.1316050

    Secondary Metabolites from an Algicolous Aspergillus versicolor Strain

    Get PDF
    Two new compounds, asperversin A (1) and 9ξ-O-2(2,3-dimethylbut-3-enyl)brevianamide Q (2), and nine known compounds, brevianamide K (3), brevianamide M (4), aversin (5), 6,8-di-O-methylnidurufin (6), 6,8-di-O-methylaverufin (7), 6-O-methylaverufin (8), 5α,8α-epidioxyergosta-6,22-dien-3β-ol (9), ergosta-7,22-diene-3β,5α,6β-triol (10), and 6β-methoxyergosta-7,22-diene-3β,5α-diol (11), were obtained from the culture of Aspergillus versicolor, an endophytic fungus isolated from the marine brown alga Sargassum thunbergii. The structures of these compounds were established by spectroscopic techniques. Compounds 4, 7 and 8 exhibited antibacterial activities against Escherichia coli and Staphyloccocus aureus, and 7 also showed lethality against brine shrimp (Artemia salina) with an LC50 value of 0.5 μg/mL

    Odorranalectin Is a Small Peptide Lectin with Potential for Drug Delivery and Targeting

    Get PDF
    BACKGROUND: Lectins are sugar-binding proteins that specifically recognize sugar complexes. Based on the specificity of protein-sugar interactions, different lectins could be used as carrier molecules to target drugs specifically to different cells which express different glycan arrays. In spite of lectin's interesting biological potential for drug targeting and delivery, a potential disadvantage of natural lectins may be large size molecules that results in immunogenicity and toxicity. Smaller peptides which can mimic the function of lectins are promising candidates for drug targeting. PRINCIPAL FINDINGS: Small peptide with lectin-like behavior was screened from amphibian skin secretions and its structure and function were studied by NMR, NMR-titration, SPR and mutant analysis. A lectin-like peptide named odorranalectin was identified from skin secretions of Odorrana grahami. It was composed of 17 aa with a sequence of YASPKCFRYPNGVLACT. L-fucose could specifically inhibit the haemagglutination induced by odorranalectin. (125)I-odorranalectin was stable in mice plasma. In experimental mouse models, odorranalectin was proved to mainly conjugate to liver, spleen and lung after i.v. administration. Odorranalectin showed extremely low toxicity and immunogenicity in mice. The small size and single disulfide bridge of odorranalectin make it easy to manipulate for developing as a drug targeting system. The cyclic peptide of odorranalectin disclosed by solution NMR study adopts a beta-turn conformation stabilized by one intramolecular disulfide bond between Cys6-Cys16 and three hydrogen bonds between Phe7-Ala15, Tyr9-Val13, Tyr9-Gly12. Residues K5, C6, F7, C16 and T17 consist of the binding site of L-fucose on odorranalectin determined by NMR titration and mutant analysis. The structure of odorranalectin in bound form is more stable than in free form. CONCLUSION: These findings identify the smallest lectin so far, and show the application potential of odorranalectin for drug delivery and targeting. It also disclosed a new strategy of amphibian anti-infection

    Incorporation of pseudouridine into mRNA enhances translation by diminishing PKR activation

    Get PDF
    Previous studies have shown that the translation level of in vitro transcribed messenger RNA (mRNA) is enhanced when its uridines are replaced with pseudouridines; however, the reason for this enhancement has not been identified. Here, we demonstrate that in vitro transcripts containing uridine activate RNA-dependent protein kinase (PKR), which then phosphorylates translation initiation factor 2-alpha (eIF-2α), and inhibits translation. In contrast, in vitro transcribed mRNAs containing pseudouridine activate PKR to a lesser degree, and translation of pseudouridine-containing mRNAs is not repressed. RNA pull-down assays demonstrate that mRNA containing uridine is bound by PKR more efficiently than mRNA with pseudouridine. Finally, the role of PKR is validated by showing that pseudouridine- and uridine-containing RNAs were translated equally in PKR knockout cells. These results indicate that the enhanced translation of mRNAs containing pseudouridine, compared to those containing uridine, is mediated by decreased activation of PKR

    Optical properties of substituted phthalocyanine rare-earth metal complexes

    Get PDF
    Comparative study of optical properties of alkylthio-group-substituted phthalocyanine rare-earth metal sandwich complexes ([(CnS)(8)Pc](2)M,M=Eu,Lu,Tb) is presented. Photoluminescence and photoconductivity of [(CnS)(8)Pc](2)M complex is very weak. Two photoluminescence bands were observed at around 400-650 and 720-800 nm in chloroform solution corresponding to the Soret and Q bands in the absorption spectra, respectively. However, the emission from Eu3+ ion (as well as Tb3+) was not found compared with other Eu complexes because the 5d levels of the Eu3+ ion lie higher than the triplet level of the ligand. The significant enhancement of the photoconductivity of [(C16S)(8)Pc](2)M after C-60 doping is reported. The photoconductivity is positive at the low electric field in the ohmic regime while it becomes negative at the high electric field upon photoexcitation with strongly absorbed light. The negative photoconductivity is attributed to space-charge effects. The mechanism of photoluminescence and photoconductivity are discussed by taking the electronic energy schemes of phthalocyanine ligands and lanthanide ion and C-60 into consideration.ArticleJOURNAL OF APPLIED PHYSICS. 88(12):7137-7143 (2000)journal articl

    Overexpression of platelet-derived growth factor receptor α in breast cancer is associated with tumour progression

    Get PDF
    INTRODUCTION: Receptor tyrosine kinases have been extensively studied owing to their frequently abnormal activation in the development and progression of human cancers. Platelet-derived growth factor receptors (PDGFRs) are receptors with intrinsic tyrosine kinase activity that regulate several functions in normal cells and are widely expressed in a variety of malignancies. After the demonstration that gastrointestinal stromal tumours without c-Kit mutations harbour PDGFR-α-activating mutations and that PDGFR-α is also a therapeutic target for imatinib mesylate, the interest for this receptor has increased considerably. Because breast cancer is one of the most frequent neoplasias in women worldwide, and only one study has reported PDGFR-α expression in breast carcinomas, the aim of this work was to investigate the potential significance of PDGFR-α expression in invasive mammary carcinomas. METHODS: We used immunohistochemistry to detect PDGFR-α overexpression on a series of 181 formalin-fixed paraffin-embedded invasive ductal breast carcinomas and in two breast cancer cell lines: MCF-7 and HS578T. We associated its expression with known prognostic factors and we also performed polymerase chain reaction–single-stranded conformational polymorphism and direct sequencing to screen for PDGFR-α mutations. RESULTS: PDGFR-α expression was observed in 39.2% of the breast carcinomas and showed an association with lymph node metastasis (P = 0.0079), HER-2 expression (P = 0.0265) and Bcl2 expression (P = 0.0121). A correlation was also found with the expression of platelet-derived growth factor A (PDGF-A; P = 0.0194). The two cell lines tested did not express PDGFR-α. Screening for mutations revealed alterations in the PDGFR-α gene at the following locations: 2500A→G, 2529T→A and 2472C→T in exon 18 and 1701G→A in exon 12. We also found an intronic insertion IVS17-50insA at exon 18 in all sequenced cases. None of these genetic alterations was correlated with PDGFR-α expression. The cell lines did not reveal any alterations in the PDGFR-α gene sequence. CONCLUSION: PDGFR-α is expressed in invasive breast carcinomas and is associated with biological aggressiveness. The genetic alterations described were not correlated with protein expression, but other mechanisms such as gene amplification or constitutive activation of a signalling pathway inducing this receptor could still sustain PDGFR-α as a potential therapeutic target
    corecore