246 research outputs found

    Inhomogeneous magnesium hydride synthesized by low temperature ion implantation: weak localization effect

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    Metastable MgHx hydride was prepared by H ion implantation into Mg films at 5 K. The resistivity and magnetoresistance temperature dependence reveal weak localization effects due to atomic disorder. At low hydrogen concentrations, x ≤0.3, the conductivity varies as σ∼log (T), typical of two-dimensional weak localization behaviour. The resistivity is also very sensitive to the sample inhomogeneity, due to H diffusion, which can be modelled by introducing a temperature-dependent geometrical percolating factor G. At higher H concentrations, 0.7 ≤x ≤3, after annealing at 20 K, 50 K and 110 K, the samples also exhibit weak localization but with three-dimensional behaviour i.e. a σT\sigma \sim \sqrt{T}. Our analysis is consistent with the existence of an inhomogeneous system formed by a mixture of two phases with contrasted conduction properties, one of which is a well-behaved metal, while the other displays the localization properties. The results lead us to identify the former phase to a non percolating superconducting phase at low temperature

    Quantum Symmetries and Strong Haagerup Inequalities

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    In this paper, we consider families of operators {xr}rΛ\{x_r\}_{r \in \Lambda} in a tracial C^\ast-probability space (A,ϕ)(\mathcal A, \phi), whose joint \ast-distribution is invariant under free complexification and the action of the hyperoctahedral quantum groups {Hn+}nN\{H_n^+\}_{n \in \N}. We prove a strong form of Haagerup's inequality for the non-self-adjoint operator algebra B\mathcal B generated by {xr}rΛ\{x_r\}_{r \in \Lambda}, which generalizes the strong Haagerup inequalities for \ast-free R-diagonal families obtained by Kemp-Speicher \cite{KeSp}. As an application of our result, we show that B\mathcal B always has the metric approximation property (MAP). We also apply our techniques to study the reduced C^\ast-algebra of the free unitary quantum group Un+U_n^+. We show that the non-self-adjoint subalgebra Bn\mathcal B_n generated by the matrix elements of the fundamental corepresentation of Un+U_n^+ has the MAP. Additionally, we prove a strong Haagerup inequality for Bn\mathcal B_n, which improves on the estimates given by Vergnioux's property RD \cite{Ve}

    Coupled pre-mRNA and mRNA dynamics unveil operational strategies underlying transcriptional responses to stimuli

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    Genome-wide simultaneous measurements of pre-mRNA and mRNA expression reveal unexpected time-dependent transcript production and degradation profiles in response to external stimulus, as well as a striking lack of concordance between mRNA abundance and transcript production profiles

    Altering an Artificial Gagpolnef Polyprotein and Mode of ENV Co-Administration Affects the Immunogenicity of a Clade C HIV DNA Vaccine

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    HIV-1 candidate vaccines expressing an artificial polyprotein comprising Gag, Pol and Nef (GPN) and a secreted envelope protein (Env) were shown in recent Phase I/II clinical trials to induce high levels of polyfunctional T cell responses; however, Env-specific responses clearly exceeded those against Gag. Here, we assess the impact of the GPN immunogen design and variations in the formulation and vaccination regimen of a combined GPN/Env DNA vaccine on the T cell responses against the various HIV proteins. Subtle modifications were introduced into the GPN gene to increase Gag expression, modify the expression ratio of Gag to PolNef and support budding of virus-like particles. I.m. administration of the various DNA constructs into BALB/c mice resulted in an up to 10-fold increase in Gag- and Pol-specific IFNγ+ CD8+ T cells compared to GPN. Co-administering Env with Gag or GPN derivatives largely abrogated Gag-specific responses. Alterations in the molar ratio of the DNA vaccines and spatially or temporally separated administration induced more balanced T cell responses. Whereas forced co-expression of Gag and Env from one plasmid induced predominantly Env-specific T cells responses, deletion of the only H-2d T cell epitope in Env allowed increased levels of Gag-specific T cells, suggesting competition at an epitope level. Our data demonstrate that the biochemical properties of an artificial polyprotein clearly influence the levels of antigen-specific T cells, and variations in formulation and schedule can overcome competition for the induction of these responses. These results are guiding the design of ongoing pre-clinical and clinical trials

    Pulmonary MR angiography and perfusion imaging—A review of methods and applications

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    The pulmonary vasculature and its role in perfusion and gas exchange is an important consideration in many conditions of the lung and heart. Currently the mainstay of imaging of the vasculature and perfusion of the lungs lies with CT and nuclear medicine perfusion scans, both of which require ionizing radiation exposure. Improvements in MRI techniques have increased the use of MRI in pulmonary vascular imaging. Here we review MRI methods for imaging the pulmonary vasculature and pulmonary perfusion, both using contrast enhanced and non-contrast enhanced methodology. In many centres pulmonary MR angiography and dynamic contrast enhanced perfusion MRI are now well established in the routine workflow of patients particularly with pulmonary hypertension and thromboembolic disease. However, these imaging modalities offer exciting new directions for future research and clinical use in other respiratory diseases where consideration of pulmonary perfusion and gas exchange can provide insight in to pathophysiology
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