594 research outputs found

    Determination of Electromagnetic Material Properties of Ferromagnetic Stainless Steel Used in Domestic Induction Heating Cookware

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    Design-oriented modeling approaches, such as finite element analyses (FEA), rely on accurate material data for the modeled hardware. In the case of cookware used in domestic induction heating (IH) systems, manufacturers rarely provide the necessary data. Therefore, this contribution presents results for the electromagnetic material properties of ferromagnetic stainless steel, typically used in cookware for domestic IH. The magnetic material properties are modeled using Jiles-Atherton hysteresis model. With the used measurement method, less effort in preparation of suited material specimen is needed compared to conventional measurement methods. The presented results for the magnetic material properties are validated using Epstein frame measurements. It is shown that the hysteresis curves are similar to each other for both measurement methods. Regarding the specific electrical resistance, the results are validated using a microhmmeter. The values determined for the specific resistance show good accordance for the different measurement methods

    Loss Comparison of Small Delta- and Star-Connected Permanent Magnet Synchronous Machines

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    Delta-connected stator windings are often used in mass production of small Permanent Magnet Synchronous Machines (PMSMs). In comparison to star-connected stator windings, a delta-connected winding system offers advantages for manufacturing and lowers production costs. A main disadvantage of motors with such a winding system are additional losses caused by the Zero-Sequence Current Component (ZSCC). In this paper the ZSCC and its impact on the generated losses in a delta-connected PMSM used as a traction motor for a pedal electric cycle (Pedelec) is analysed. The calculated results are compared to those of a star-connected PMSM with the same design. We will show that the amplitude of the ZSCC depends on the operating point of the machine. As a result, the copper losses in the delta-connected machine are up to 5.8 % higher than the ones in the star-connected machine. On the other hand, the iron losses are 1 % smaller in the delta-connected machine. The efficiency of the delta-connected machine is still up to 4 % smaller

    Linear approaches to intramolecular Förster Resonance Energy Transfer probe measurements for quantitative modeling

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    Numerous unimolecular, genetically-encoded Forster Resonance Energy Transfer (FRET) probes for monitoring biochemical activities in live cells have been developed over the past decade. As these probes allow for collection of high frequency, spatially resolved data on signaling events in live cells and tissues, they are an attractive technology for obtaining data to develop quantitative, mathematical models of spatiotemporal signaling dynamics. However, to be useful for such purposes the observed FRET from such probes should be related to a biological quantity of interest through a defined mathematical relationship, which is straightforward when this relationship is linear, and can be difficult otherwise. First, we show that only in rare circumstances is the observed FRET linearly proportional to a biochemical activity. Therefore in most cases FRET measurements should only be compared either to explicitly modeled probes or to concentrations of products of the biochemical activity, but not to activities themselves. Importantly, we find that FRET measured by standard intensity-based, ratiometric methods is inherently non-linear with respect to the fraction of probes undergoing FRET. Alternatively, we find that quantifying FRET either via (1) fluorescence lifetime imaging (FLIM) or (2) ratiometric methods where the donor emission intensity is divided by the directly-excited acceptor emission intensity (denoted R<sub>alt</sub>) is linear with respect to the fraction of probes undergoing FRET. This linearity property allows one to calculate the fraction of active probes based on the FRET measurement. Thus, our results suggest that either FLIM or ratiometric methods based on R<sub>alt</sub> are the preferred techniques for obtaining quantitative data from FRET probe experiments for mathematical modeling purpose

    International federation of genomic medicine databases using GA4GH standards

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    We promote a shared vision and guide for how and when to federate genomic and health-related data sharing, enabling connections and insights across independent, secure databases. The GA4GH encourages a federated approach wherein data providers have the mandate and resources to share, but where data cannot move for legal or technical reasons. We recommend a federated approach to connect national genomics initiatives into a global network and precision medicine resource

    Catching Element Formation In The Act

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    Gamma-ray astronomy explores the most energetic photons in nature to address some of the most pressing puzzles in contemporary astrophysics. It encompasses a wide range of objects and phenomena: stars, supernovae, novae, neutron stars, stellar-mass black holes, nucleosynthesis, the interstellar medium, cosmic rays and relativistic-particle acceleration, and the evolution of galaxies. MeV gamma-rays provide a unique probe of nuclear processes in astronomy, directly measuring radioactive decay, nuclear de-excitation, and positron annihilation. The substantial information carried by gamma-ray photons allows us to see deeper into these objects, the bulk of the power is often emitted at gamma-ray energies, and radioactivity provides a natural physical clock that adds unique information. New science will be driven by time-domain population studies at gamma-ray energies. This science is enabled by next-generation gamma-ray instruments with one to two orders of magnitude better sensitivity, larger sky coverage, and faster cadence than all previous gamma-ray instruments. This transformative capability permits: (a) the accurate identification of the gamma-ray emitting objects and correlations with observations taken at other wavelengths and with other messengers; (b) construction of new gamma-ray maps of the Milky Way and other nearby galaxies where extended regions are distinguished from point sources; and (c) considerable serendipitous science of scarce events -- nearby neutron star mergers, for example. Advances in technology push the performance of new gamma-ray instruments to address a wide set of astrophysical questions.Comment: 14 pages including 3 figure

    Research Directions in the Clinical Implementation of Pharmacogenomics: An Overview of US Programs and Projects

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    Response to a drug often differs widely among individual patients. This variability is frequently observed not only with respect to effective responses but also with adverse drug reactions. Matching patients to the drugs that are most likely to be effective and least likely to cause harm is the goal of effective therapeutics. Pharmacogenomics (PGx) holds the promise of precision medicine through elucidating the genetic determinants responsible for pharmacological outcomes and using them to guide drug selection and dosing. Here we survey the US landscape of research programs in PGx implementation, review current advances and clinical applications of PGx, summarize the obstacles that have hindered PGx implementation, and identify the critical knowledge gaps and possible studies needed to help to address them

    ACMG recommendations for reporting of incidental findings in clinical exome and genome sequencing

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    In clinical exome and genome sequencing, there is potential for the recognition and reporting of incidental or secondary findings unrelated to the indication for ordering the sequencing but of medical value for patient care. The American College of Medical Genetics and Genomics (ACMG) recently published a policy statement on clinical sequencing, which emphasized the importance of disclosing the possibility of such results in pretest patient discussions, clinical testing, and reporting of results. The ACMG appointed a Working Group on Incidental Findings in Clinical Exome and Genome Sequencing to make recommendations about responsible management of incidental findings when patients undergo exome or genome sequencing. This Working Group conducted a year-long consensus process, including review by outside experts, and produced recommendations that have been approved by the ACMG Board. Specific and detailed recommendations, and the background and rationale for these recommendations, are described herein. We recommend that laboratories performing clinical sequencing seek and report mutations of the specified classes or types in the genes listed here. This evaluation and reporting should be performed for all clinical germline (constitutional) exome and genome sequencing, including the ‘normal’ of tumor-normal subtractive analyses in all subjects, irrespective of age, but excluding fetal samples. We recognize that there are insufficient data on clinical utility to fully support these recommendations and we encourage the creation of an ongoing process for updating these recommendations at least annually as further data are collected
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