294 research outputs found

    EXPLORANDO A ESPIRAL DE ARQUIMEDES COM SOFTWARE DE GEOMETRIA DINÂMICA

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    Este artigo apresenta análise e discussão de uma investigação realizada com estudantes do Ensino Médio na cidade de Macapá, no Estado do Amapá. Teve como objetivo explorar a construção da Espiral de Arquimedes no ambiente do software Geogebra e desenvolver a atividade de calcular o comprimento e o número de voltas de papel constantes de uma bobina utilizada para armazená-lo. A metodologia utilizada foi a investigação matemática e, para realizá-la, os investigadores planejaram e aplicaram uma sequência de passos orientadores para a resolução, a qual teve como instrumento de apoio o Geogebra. Os resultados da investigação mostraram que os alunos investigados conseguiram modelar uma bobina e calcular o número de voltas de papel que a mesma contém, bem como o seu comprimento. Por sua vez, os depoimentos dos estudantes mostraram que a utilização da metodologia e do software foram incentivadores para a aprendizagem e sugeriram ao professor titular empregá-la em outros conteúdos

    Microbes as engines of ecosystem function : When does community structure enhance predictions of ecosystem processes?

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    FUNDING This work was supported by NSF grant DEB-1221215 to DN, as well as grants supporting the generation of our datasets as acknowledged in their original publications and in Supplementary Table S1. ACKNOWLEDGMENT We thank the USGS Powell Center ‘Next Generation Microbes’ working group, anonymous reviews, Brett Melbourne, and Alan Townsend for valuable feedback on this project.Peer reviewedPublisher PD

    Assay strategies for the discovery and validation of therapeutics targeting <i>Brugia pahangi</i> Hsp90

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    The chemotherapy of lymphatic filariasis relies upon drugs such as diethylcarbamazine and ivermectin that largely target the microfilarial stages of the parasite, necessitating continued treatment over the long reproductive life span of the adult worm. The identification of compounds that target adult worms has been a long-term goal of WHO. Here we describe a fluorescence polarization assay for the identification of compounds that target Hsp90 in adult filarial worms. The assay was originally developed to identify inhibitors of Hsp90 in tumor cells, and relies upon the ability of small molecules to inhibit the binding of fluorescently labelled geldanamycin to Hsp90. We demonstrate that the assay works well with soluble extracts of Brugia, while extracts of the free-living nematode C. elegans fail to bind the probe, in agreement with data from other experiments. The assay was validated using known inhibitors of Hsp90 that compete with geldanamycin for binding to Hsp90, including members of the synthetic purine-scaffold series of compounds. The efficacy of some of these compounds against adult worms was confirmed in vitro. Moreover, the assay is sufficiently sensitive to differentiate between binding of purine-scaffold compounds to human and Brugia Hsp90. The assay is suitable for high-throughput screening and provides the first example of a format with the potential to identify novel inhibitors of Hsp90 in filarial worms and in other parasitic species where Hsp90 may be a target

    GPML: an XML-based standard for the interchange of genetic programming trees

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    We propose a Genetic Programming Markup Language (GPML), an XML based standard for the interchange of genetic programming trees, and outline the benefits such a format would bring in allowing the deployment of trained genetic programming (GP) models in applications as well as the subsidiary benefit of allowing GP researchers to directly share trained trees. We present a formal definition of this standard and describe details of an implementation. In addition, we present a case study where GPML is used to implement a model predictive controller for the control of a building heating plant

    A rare case: paratesticular leiomyosarcoma

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    The role of released ATP in killing Candida albicans and other extracellular microbial pathogens by cationic peptides

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    A unifying theme common to the action of many cationic peptides that display lethal activities against microbial pathogens is their specific action at microbial membranes that results in selective loss of ions and small nucleotides chiefly ATP. One model cationic peptide that induces non-lytic release of ATP from the fungal pathogen Candida albicans is salivary histatin 5 (Hst 5). The major characteristic of Hst 5-induced ATP release is that it occurs rapidly while cells are still metabolically active and have polarized membranes, thus precluding cell lysis as the means of release of ATP. Other cationic peptides that induce selective release of ATP from target microbes are lactoferricin, human neutrophil defensins, bactenecin, and cathelicidin peptides. The role of released extracellular ATP induced by cationic peptides is not known, but localized increases in extracellular ATP concentration may serve to potentiate cell killing, facilitate further peptide uptake, or function as an additional signal to activate the host innate immune system at the site of infection
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