449 research outputs found

    Amplifier provides dual outputs from a single source with complete isolation

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    Amplifier provides two amplified outputs from a single input signal with complete transformer isolation. It uses modulation techniques to obtain the separated output

    Offsetting of CO₂ emissions by air capture in mine tailings at the Mount Keith Nickel Mine, Western Australia: Rates, controls and prospects for carbon neutral mining

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    The hydrated Mg-carbonate mineral, hydromagnesite [Mg₅(CO₃)₄(OH)₂•4H₂O], precipitates within mine tailings at the Mount Keith Nickel Mine, Western Australia as a direct result of mining operations. We have used quantitative mineralogical data and δ¹³C, δ¹⁸O and F¹⁴C isotopic data to quantify the amount of CO₂fixation and identify carbon sources. Our radiocarbon results indicate that at least 80% of carbon stored in hydromagnesite has been captured from the modern atmosphere. Stable isotopic results indicate that dissolution of atmospheric CO₂ into mine tailings water is kinetically limited, which suggests that the current rate of carbon mineralization could be accelerated. Reactive transport modeling is used to describe the observed variation in tailings mineralogy and to estimate rates of CO₂ fixation. Based on our assessment, approximately 39,800 t/yr of atmospheric CO₂ are being trapped and stored in tailings at Mount Keith. This represents an offsetting of approximately 11% of the mine's annual greenhouse gas emissions. Thus, passive sequestration via enhanced weathering of mineral waste can capture and store a significant amount of CO₂. Recommendations are made for changes to tailings management and ore processing practices that have potential to accelerate carbonation of tailings and further reduce or completely offset the net greenhouse gas emissions at Mount Keith and many other mines

    The crystal structure of stichtite, re-examination of barbertonite, and the nature of polytypism in MgCr hydrotalcites

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    abStraCt Stichtite, ideally Mg 6 Cr 2 CO 3 (OH) 16 •4H 2 O, from Stichtite Hill, Tasmania, Australia, and barbertonite, also ideally Mg 6 Cr 2 CO 3 (OH) 16 •4H 2 O, from the Kaapsehoop asbestos mine, South Africa, have been studied by powder X-ray diffraction and their structures have been refined using the Rietveld method. Stichtite from Stichtite Hill crystallizes in the rhombohedral space group R3m, with unitcell parameters a = 3.09575(3) and c = 23.5069(6) Å, V = 195.099(6) Å 3 , with Z = 3/8. Barbertonite from the Kaapsehoop asbestos mine crystallizes in the hexagonal space group P6 3 /mmc. The co-type specimens of barbertonite were found to be intergrown mixtures consisting of barbertonite and stichtite. Unit-cell parameters of barbertonite from the co-type specimens were a = 3.09689(6), c = 15.6193(8) Å, and V = 129.731(8) Å 3 and a = 3.09646(6), c = 15.627(1) Å V = 129.76(1) Å 3 , and Z = ¼. Rietveld refinements of both stichtite and barbertonite show that they are polytypes rather than polymorphs and do not represent distinct mineral species. Several possible nomenclature systems are discussed for the naming of hydrotalcite minerals and groups. Raman band assignments are also presented for stichtite from Stichtite Hill. Stichtite and hydrotalcite minerals make up a large proportion of the ore at the Mount Keith nickel mine in Western Australia. Bulk powder diffraction shows the ore contains 6.1 wt% stichtite and 5.6 wt% iowaite. Hydrotalcite group minerals provide an important potential reservoir of CO 2 . At Mount Keith, the amount of CO 2 mined as stichtite could exceed 45 000 metric tons per year, while exchange of Cl for CO 3 could fix in excess of 40 000 metric tons CO 2 per year if end-member iowaite is reacted to form pyaroaurite

    Dominant-negative variant in SLC1A4 causes an autosomal dominant epilepsy syndrome.

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    SLC1A4 is a trimeric neutral amino acid transporter essential for shuttling L-serine from astrocytes into neurons. Individuals with biallelic variants in SLC1A4 are known to have spastic tetraplegia, thin corpus callosum, and progressive microcephaly (SPATCCM) syndrome, but individuals with heterozygous variants are not thought to have disease. We identify an 8-year-old patient with global developmental delay, spasticity, epilepsy, and microcephaly who has a de novo heterozygous three amino acid duplication in SLC1A4 (L86_M88dup). We demonstrate that L86_M88dup causes a dominant-negative N-glycosylation defect of SLC1A4, which in turn reduces the plasma membrane localization of SLC1A4 and the transport rate of SLC1A4 for L-serine

    Disease-associated pathophysiologic structures in pediatric rheumatic diseases show characteristics of scale-free networks seen in physiologic systems: implications for pathogenesis and treatment

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    <p>Abstract</p> <p>Background</p> <p>While standard reductionist approaches have provided some insights into specific gene polymorphisms and molecular pathways involved in disease pathogenesis, our understanding of complex traits such as atherosclerosis or type 2 diabetes remains incomplete. Gene expression profiling provides an unprecedented opportunity to understand complex human diseases by providing a global view of the multiple interactions across the genome that are likely to contribute to disease pathogenesis. Thus, the goal of gene expression profiling is not to generate lists of differentially expressed genes, but to identify the physiologic or pathogenic processes and structures represented in the expression profile.</p> <p>Methods</p> <p>RNA was separately extracted from peripheral blood neutrophils and mononuclear leukocytes, labeled, and hybridized to genome level microarrays to generate expression profiles of children with polyarticular juvenile idiopathic arthritis, juvenile dermatomyositis relative to childhood controls. Statistically significantly differentially expressed genes were identified from samples of each disease relative to controls. Functional network analysis identified interactions between products of these differentially expressed genes.</p> <p>Results</p> <p><it>In silico </it>models of both diseases demonstrated similar features with properties of scale-free networks previously described in physiologic systems. These networks were observable in both cells of the innate immune system (neutrophils) and cells of the adaptive immune system (peripheral blood mononuclear cells).</p> <p>Conclusion</p> <p>Genome-level transcriptional profiling from childhood onset rheumatic diseases suggested complex interactions in two arms of the immune system in both diseases. The disease associated networks showed scale-free network patterns similar to those reported in normal physiology. We postulate that these features have important implications for therapy as such networks are relatively resistant to perturbation.</p
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