383 research outputs found

    Simulation of Internal Undular Bores Propagating over a Slowly Varying Region

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    Internal undular bores have been observed in many parts of the world. Studies have shown that many marine structures face danger and risk of destruction caused by internal undular bores due to the amount of energy it carries. This paper looks at the transformation of internal undular bore in two-layer fluid flow under the influence of variable topography. Thus, the surface of the bottom is considered to be slowly varying. The appropriate mathematical model is the variable-coefficient extended Korteweg-de Vries equation. We are particularly interested in looking at the transformation of KdV-type and table-top undular bore over the variable topography region. The governing equation is solved numerically using the method of lines, where the spatial derivatives are first discretised using finite difference approximation so that the partial differential equation becomes a system of ordinary differential equations which is then solved by 4th order Runge-Kutta method. Our numerical results show that the evolution of internal undular bore over different types of varying depths regions leads to a number of adiabatic and non-adiabatic effects. When the depth decreases slowly, a solitary wavetrain is observed at the front of the transformed internal undular bore. On the other hand, when the depth increases slowly, we observe the generation of step-like wave and weakly nonlinear trailing wavetrain, the occurrence of multi-phase behaviour, the generation of transformed undular bore of negative polarity and diminishing transformed undular bore depending on the nature of the topography after the variable topography

    A chamber experiment for the feasibility study of an artificial plasma reflector for OTH radar applications

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    The feasibility of using two intersecting beams for plasma generation in the upper atmosphere as an over-the-horizon radar reflector was investigated. A cube was filled with dry air to a pressure corresponding to the simulated altitude, and two components of a split microwave beam were fed into the cube at right angles. Plasma layers were generated where the two beams intersected. Three critical issues were addressed: (1) reflectivity of the generated plasma layers; (2) propagation of high power microwave pulses; and (3) lifetime of the plasma

    Moth flame optimization maximum power point tracking algorithm for photovoltaic system under partial shaded conditions

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    This paper presents a study in maximum power point tracking (MPPT) technique in solar photovoltaic (PV) using moth flame optimization (MFO) algorithm. Despite the solar PV is one of the most popular method for power generation, the effort to maximize the energy yield from the installed PV system remains a challenge. The study aims to identify the performance of MFO based MPPT algorithm under partial shaded conditions. A simulation model of MFO based MPPT algorithm was developed and implemented with DC/DC boost converter in MATLAB Simulink. For comparison, a well-established particle swarm optimization (PSO) algorithm was included in the study. Both MPPT algorithms were examined under MATLAB simulation as well as real-time hardware-in-the-loop (HIL) platform using HIL emulator and digital signal processing (DSP) card. Under 10 partial shaded condition test cases, the MFO has shown its capability in tracking for the maximum power operating point effectively, with zero steady state oscillation. Both algorithms in study have shown their capability in tracking for maximum power operating point with output efficiency up to 99% in both simulation and real-time platform

    Local structure evolution in polycrystalline Zn1βˆ’x_{1-x}Mgx_xO (0≀x≀0.150\leq{x}\leq{0.15}) studied by Raman and by synchrotron x-ray pair distribution analysis

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    The local structures of Zn1βˆ’x_{1-x}Mgx_xO alloys have been studied by Raman spectroscopy and by synchrotron x-ray pair distribution function (PDF) analysis. Within the solid solution range (0≀x≀0.150\leq{x}\leq{0.15}) of Zn1βˆ’x_{1-x}Mgx_xO, the wurtzite framework is maintained with Mg homogeneously distributed throughout the wurtzite lattice. The E2highE_2^\mathrm{high} Raman line of Zn1βˆ’x_{1-x}Mgx_xO displays systematic changes in response to the evolution of the crystal lattice upon the Mg-substitution. The red-shift and broadening of the E2highE_2^\mathrm{high} mode are explained by the expansion of hexagonal abab-dimensions, and compositional disorder of Zn/Mg, respectively. Synchrotron x-ray PDF analyses of Zn1βˆ’x_{1-x}Mgx_xO reveal that the Mg atoms have a slightly reduced wurtzite parameter uu and more regular tetrahedral bond distances than the Zn atoms. For both Zn and Mg, the internal tetrahedral geometries are independent of the alloy composition.Comment: 10 pages, 12 figures RevTe

    A putative relay circuit providing low-threshold mechanoreceptive input to lamina I projection neurons via vertical cells in lamina II of the rat dorsal horn

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    Background: Lamina I projection neurons respond to painful stimuli, and some are also activated by touch or hair movement. Neuropathic pain resulting from peripheral nerve damage is often associated with tactile allodynia (touch-evoked pain), and this may result from increased responsiveness of lamina I projection neurons to non-noxious mechanical stimuli. It is thought that polysynaptic pathways involving excitatory interneurons can transmit tactile inputs to lamina I projection neurons, but that these are normally suppressed by inhibitory interneurons. Vertical cells in lamina II provide a potential route through which tactile stimuli can activate lamina I projection neurons, since their dendrites extend into the region where tactile afferents terminate, while their axons can innervate the projection cells. The aim of this study was to determine whether vertical cell dendrites were contacted by the central terminals of low-threshold mechanoreceptive primary afferents. Results: We initially demonstrated contacts between dendritic spines of vertical cells that had been recorded in spinal cord slices and axonal boutons containing the vesicular glutamate transporter 1 (VGLUT1), which is expressed by myelinated low-threshold mechanoreceptive afferents. To confirm that the VGLUT1 boutons included primary afferents, we then examined vertical cells recorded in rats that had received injections of cholera toxin B subunit (CTb) into the sciatic nerve. We found that over half of the VGLUT1 boutons contacting the vertical cells were CTb-immunoreactive, indicating that they were of primary afferent origin. Conclusions: These results show that vertical cell dendritic spines are frequently contacted by the central terminals of myelinated low-threshold mechanoreceptive afferents. Since dendritic spines are associated with excitatory synapses, it is likely that most of these contacts were synaptic. Vertical cells in lamina II are therefore a potential route through which tactile afferents can activate lamina I projection neurons, and this pathway could play a role in tactile allodynia

    The Drosophila Mitochondrial Translation Elongation Factor G1 Contains a Nuclear Localization Signal and Inhibits Growth and DPP Signaling

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    Mutations in the human mitochondrial elongation factor G1 (EF-G1) are recessive lethal and cause death shortly after birth. We have isolated mutations in iconoclast (ico), which encodes the highly conserved Drosophila orthologue of EF-G1. We find that EF-G1 is essential during fly development, but its function is not required in every tissue. In contrast to null mutations, missense mutations exhibit stronger, possibly neomorphic phenotypes that lead to premature death during embryogenesis. Our experiments show that EF-G1 contains a secondary C-terminal nuclear localization signal. Expression of missense mutant forms of EF-G1 can accumulate in the nucleus and cause growth and patterning defects and animal lethality. We find that transgenes that encode mutant human EF-G1 proteins can rescue ico mutants, indicating that the underlying problem of the human disease is not just the loss of enzymatic activity. Our results are consistent with a model where EF-G1 acts as a retrograde signal from mitochondria to the nucleus to slow down cell proliferation if mitochondrial energy output is low

    Pathogenic variants in the paired-related homeobox 1 gene (PRRX1) cause craniosynostosis with incomplete penetrance

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    Purpose Studies previously implicated PRRX1 in craniofacial development, including demonstration of murine Prrx1 expression in the pre-osteogenic cells of the cranial sutures. We investigated the role of heterozygous missense and loss-of-function variants in PRRX1 associated with craniosynostosis. Methods Trio-based genome, exome or targeted sequencing were used to screen PRRX1 in patients with craniosynostosis; immunofluorescence analyses were used to assess nuclear localization of wild-type and mutant proteins. Results Genome sequencing identified 2 of 9 sporadically affected individuals with syndromic/multisuture craniosynostosis who were heterozygous for rare/undescribed variants in PRRX1. Exome or targeted sequencing of PRRX1 revealed a further 9/1449 patients with craniosynostosis harboring deletions or rare heterozygous variants within the homeodomain. By collaboration, seven additional individuals (four families) were identified with putatively pathogenic PRRX1 variants. Immunofluorescence analyses showed that missense variants within the PRRX1 homeodomain cause abnormal nuclear localization. Of patients with variants considered likely pathogenic, bicoronal or other multi-suture synostosis was present in 11/17 (65% of the cases). Pathogenic variants were inherited from unaffected relatives in many instances, yielding a 12.5% penetrance estimate for craniosynostosis. Conclusion This work supports a key role for PRRX1 in cranial suture development and shows that haploinsufficiency of PRRX1 is a relatively frequent cause of craniosynostosis

    In Vivo Mapping of Vascular Inflammation Using Multimodal Imaging

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    Plaque vulnerability to rupture has emerged as a critical correlate to risk of adverse coronary events but there is as yet no clinical method to assess plaque stability in vivo. In the search to identify biomarkers of vulnerable plaques an association has been found between macrophages and plaque stability--the density and pattern of macrophage localization in lesions is indicative of probability to rupture. In very unstable plaques, macrophages are found in high densities and concentrated in the plaque shoulders. Therefore, the ability to map macrophages in plaques could allow noninvasive assessment of plaque stability. We use a multimodality imaging approach to noninvasively map the distribution of macrophages in vivo. The use of multiple modalities allows us to combine the complementary strengths of each modality to better visualize features of interest. Our combined use of Positron Emission Tomography and Magnetic Resonance Imaging (PET/MRI) allows high sensitivity PET screening to identify putative lesions in a whole body view, and high resolution MRI for detailed mapping of biomarker expression in the lesions.Macromolecular and nanoparticle contrast agents targeted to macrophages were developed and tested in three different mouse and rat models of atherosclerosis in which inflamed vascular plaques form spontaneously and/or are induced by injury. For multimodal detection, the probes were designed to contain gadolinium (T1 MRI) or iron oxide (T2 MRI), and Cu-64 (PET). PET imaging was utilized to identify regions of macrophage accumulation; these regions were further probed by MRI to visualize macrophage distribution at high resolution. In both PET and MR images the probes enhanced contrast at sites of vascular inflammation, but not in normal vessel walls. MRI was able to identify discrete sites of inflammation that were blurred together at the low resolution of PET. Macrophage content in the lesions was confirmed by histology.The multimodal imaging approach allowed high-sensitivity and high-resolution mapping of biomarker distribution and may lead to a clinical method to predict plaque probability to rupture
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