3,730 research outputs found

    The Electrochemical Oxidation of Substituted Catechols

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    The oxidation of substituted catechols was studied by cyclic voltammetry, chronoamperometry, rotating ring‐disk electrode, and coulometry. The results showed that the quinones that were formed from the oxidation of substituted catechols reacted with the basic forms of the starting material to yield the dimeric product. These products were generally unstable and rapidly polymerized or underwent some other irreversible reaction to form an electroinactive product. For 3,4‐dihydroxyacetophenone and propriophenone, the intermediate was stable long enough to be observed in cyclic voltammetry. The rate of the coupling reaction was found to correlate well with the Hammett ρ‐σ parameters and indicated that there was substantial negative charge in the transition state. Finally, an analysis of the coulometric n‐values along with the iat1/2/C values indicated that the initial coupling product was a diphenyl ether. Analysis of the coulometry products showed extensive polymerization

    Tailored design of NKT-stimulatory glycolipids for polarization of immune responses.

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    Natural killer T (NKT) cell is a distinct population of T lymphocytes that can rapidly release massive amount of Th1 and Th2 cytokines upon the engagement of their T cell receptor with glycolipids presented by CD1d. The secreted cytokines can promote cell-mediated immunity to kill tumor cells and intracellular pathogens, or suppress autoreactive immune cells in autoimmune diseases. Thus, NKT cell is an attractive target for developing new therapeutics to manipulate immune system. The best-known glycolipid to activate NKT cells is α-galactosylceramide (α-GalCer), which has been used as a prototype for designing new NKT stimulatory glycolipids. Many analogues have been generated by modification of the galactosyl moiety, the acyl chain or the phytosphingosine chain of α-GalCer. Some of the analogues showed greater abilities than α-GalCer in polarizing immune responses toward Th1 or Th2 dominance. Among them, several analogues containing phenyl groups in the lipid tails were more potent in inducing Th1-skewed cytokines and exhibited greater anticancer efficacy than α-GalCer. Analyses of the correlation between structure and activity of various α-GalCer analogues on the activation of iNKT cell revealed that CD1d-glycolipid complexes interacted with the same population of iNKT cell expressing similar T-cell receptor VÎČ as α-GalCer. On the other hand, those phenyl glycolipids with propensity for Th1 dominant responses showed greater binding avidity and stability than α-GalCer for iNKT T-cell receptor when complexed with CD1d. Thus, it is the avidity and stability of the ternary complexes of CD1d-glycolipid-iNKT TCR that dictate the polarity and potency of immune responses. These findings provide a key to the rationale design of immune modulating glycolipids with desirable Th1/Th2 polarity for clinical application. In addition, elucidation of α-GalCer-induced anergy, liver damage and accumulation of myeloid derived suppressor cells has offered explanation for its lacklustre anti-cancer activities in clinical trials. On other hand, the lack of such drawbacks in glycolipid analogues containing phenyl groups in the lipid tails of α-GalCer coupled with the greater binding avidity and stability of CD1d-glycolipid complex for iNKT T-cell receptor, account for their superior anti-cancer efficacy in tumor bearing mice. Further clinical development of these phenyl glycolipids is warranted

    Timed Fault Tree Models of the China Yongwen Railway Accident

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    Safety is an essential requirement for railway transportation. There are many methods that have been developed to predict, prevent and mitigate accidents in this context. All of these methods have their own purpose and limitations. This paper presents a new useful analysis technique: timed fault tree analysis. This method extends traditional fault tree analysis with temporal events and fault characteristics. Timed Fault Trees (TFTs) can determine which faults need to be eliminated urgently, and it can also provide a safe time window to repair them. They can also be used to determine the time taken for railway maintenance requirements, and thereby improve maintenance efficiency, and reduce risks. In this paper, we present the features and functionality of a railway transportation system based on timed fault tree models. We demonstrate the applicability of our framework via a case study of the China Yongwen line railway accident

    Biological effects of cigarette smoke in cultured human retinal pigment epithelial cells.

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    The goal of the present study was to determine whether treatment with cigarette smoke extract (CSE) induces cell loss, cellular senescence, and extracellular matrix (ECM) synthesis in primary human retinal pigment epithelial (RPE) cells. Primary cultured human RPE cells were exposed to 2, 4, 8, and 12% of CSE concentration for 24 hours. Cell loss was detected by cell viability assay. Lipid peroxidation was assessed by loss of cis-parinaric acid (PNA) fluorescence. Senescence-associated ß-galactosidase (SA-ß-Gal) activity was detected by histochemical staining. Expression of apolipoprotein J (Apo J), connective tissue growth factor (CTGF), fibronectin, and laminin were examined by real-time PCR, western blot, or ELISA experiments. The results showed that exposure of cells to 12% of CSE concentration induced cell death, while treatment of cells with 2, 4, and 8% CSE increased lipid peroxidation. Exposure to 8% of CSE markedly increased the number of SA-ß-Gal positive cells to up to 82%, and the mRNA expression of Apo J, CTGF, and fibronectin by approximately 3-4 fold. Treatment with 8% of CSE also increased the protein expression of Apo J and CTGF and the secretion of fibronectin and laminin. Thus, treatment with CSE can induce cell loss, senescent changes, and ECM synthesis in primary human RPE cells. It may be speculated that cigarette smoke could be involved in cellular events in RPE cells as seen in age-related macular degeneration

    A Vertical Resonance Heating Model for X- or Peanut-Shaped Galactic Bulges

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    We explore a second order Hamiltonian vertical resonance model for X-shaped or peanut-shaped galactic bulges. The X-shape is caused by the 2:1 vertical Lindblad resonance with the bar, with two vertical oscillation periods per orbital period in the bar frame. We examine N-body simulations and find that due to the bar slowing down and disk thickening during bar buckling, the resonance and associated peanut-shape moves outward. The peanut-shape is consistent with the location of the vertical resonance, independent of whether the bar buckled or not. We estimate the resonance width from the potential m=4 Fourier component and find that the resonance is narrow, affecting orbits over a narrow range in the angular momentum distribution, dL/L ~ 0.05. As the resonance moves outward, stars originally in the mid plane are forced out of the mid plane into orbits just within the resonance separatrix. The height of the separatrix orbits, estimated from the Hamiltonian model, is approximately consistent with the peanut-shape height. The X-shape is comprised of stars in the vicinity of the resonance separatrix. The velocity distributions from the simulations illustrate that low inclination orbits are depleted within resonance. Within resonance, the vertical velocity distribution is broad, consistent with resonant heating caused by the passage of the resonance through the disk. In the Milky Way bulge we relate the azimuthally averaged mid-plane mass density near the vertical resonance to the rotation curve and bar pattern speed. At an estimated vertical resonance galactocentric radius of ~1.3 kpc, we confirm a mid-plane density of ~5x10^8 Msol/kpc^3, consistent with recently estimated mass distributions. We find that the rotation curve, bar pattern speed, 2:1 vertical resonance location, X-shape tips, and mid-plane mass density, are all self-consistent in the Milky Way galaxy bulge.Comment: accepted for publication in MNRA
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