38 research outputs found

    Concurrent Outbreak of Norovirus Genotype I and Enterotoxigenic Escherichia coli on a U.S. Navy Ship following a Visit to Lima, Peru

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    An outbreak of norovirus (NoV) genotype I and Enterotoxigenic Escherichia coli (ETEC) occurred among US Navy Ship personnel following a visit to Lima, Peru, in June 2008. Visiting a specific area in Lima was significantly associated with illness. While ETEC and NoV are commonly recognized as causative agents of outbreaks, co-circulation of both pathogens has been rarely observed in shipboard outbreaks

    Neuroanatomy and cadaver dissection in Italy: History, medicolegal issues, and neurosurgical perspectives.

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    Despite the significant Italian tradition of important anatomical studies, an outdated law historically influenced by the Catholic church restricts the use of cadavers for teaching and scientific purposes. The object of the present paper was to trace the historical evolution of the Italian anatomical tradition, particularly neuroanatomical studies, in relation to the juridical regulations on the use of cadavers today. Special attention was paid to the opportunities offered to neurosurgery by using cadavers and to the scientific and social issues in neurosurgical training in the twenty-first century. Considering the new Common European Constitution, the authors advocate a political solution from the European community to improve the quality of training in the disciplines with a social impact such as neurosurgery

    Mild cognitive impairment is associated with poor physical function but not bone structure or density in late adulthood:Findings from the Hertfordshire Cohort Study

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    Mini Abstract This study investigated the association between mild cognitive impairment (MCI) and physical function and bone health in older adults. MCI was associated with poor physical performance but not bone mineral density or bone microarchitecture. Abstract Purpose: Cross-sectional study to investigate the association between mild cognitive impairment (MCI) and physical performance, and bone health, in a community-dwelling cohort of older adults. Methods: Cognitive function of 222 men and 221 women (mean age 75.5 and 75.8 years in men and women, respectively) was assessed by the Strawbridge questionnaire and Mini Mental State Exam (MMSE). Participants underwent dual-energy x-ray absorptiometry (DXA), peripheral-quantitative computed tomography (pQCT) and high-resolution peripheral-quantitative computed tomography (HR-pQCT) scans to assess their bone density, strength and microarchitecture. Their physical function was assessed and a physical performance (PP) score was recorded. Results: 11.8% of women and 8.1% of men in the study were cognitive impaired on the MMSE (score<24). 24% of women were deemed cognitively impaired on the Strawbridge questionnaire, compared to 22.3% of men. Cognitive impairment on the Strawbridge questionnaire was associated with poorer physical performance score in men but not women in the unadjusted analysis. MMSE <24 was strongly associated with the risk of low physical performance in men (OR 12.9, 95% CI 1.67, 99.8, p=0.01) Higher MMSE score was associated with better physical performance in both sexes. Poorer cognitive function, whether assessed by the Strawbridge questionnaire, or by MMSE score, was not associated with bone density, shape or microarchitecture, in either sex. Conclusion: MCI in older adults was associated with poor physical performance, but not bone density, shape or microarchitecture

    Eugenia punicifolia leaf extract has a hypotensive effect and inhibits angiotensin-converting enzyme activity in both in vitro and in vivo models.

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    Chronic high blood pressure has for many years been considered a public health problem. Eugenia punicifolia is a plant used to treat diabetes by the local population, however its hypotensive effect has never been investigated

    A New Method for the Characterization of Strain-Specific Conformational Stability of Protease-Sensitive and Protease-Resistant PrPSc

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    Although proteinacious in nature, prions exist as strains with specific self-perpetuating biological properties. Prion strains are thought to be associated with different conformers of PrPSc, a disease-associated isoform of the host-encoded cellular protein (PrPC). Molecular strain typing approaches have been developed which rely on the characterization of protease-resistant PrPSc. However, PrPSc is composed not only of protease-resistant but also of protease-sensitive isoforms. The aim of this work was to develop a protocol for the molecular characterization of both, protease-resistant and protease-sensitive PrPSc aggregates. We first set up experimental conditions which allowed the most advantageous separation of PrPC and PrPSc by means of differential centrifugation. The conformational solubility and stability assay (CSSA) was then developed by measuring PrPSc solubility as a function of increased exposure to GdnHCl. Brain homogenates from voles infected with human and sheep prion isolates were analysed by CSSA and showed strain-specific conformational stabilities, with mean [GdnHCl]1/2 values ranging from 1.6 M for MM2 sCJD to 2.1 for scrapie and to 2.8 M for MM1/MV1 sCJD and E200K gCJD. Interestingly, the rank order of [GdnHCl]1/2 values observed in the human and sheep isolates used as inocula closely matched those found following transmission in voles, being MM1 sCJD the most resistant (3.3 M), followed by sheep scrapie (2.2 M) and by MM2 sCJD (1.6 M). In order to test the ability of CSSA to characterise protease-sensitive PrPSc, we analysed sheep isolates of Nor98 and compared them to classical scrapie isolates. In Nor98, insoluble PrPSc aggregates were mainly protease-sensitive and showed a conformational stability much lower than in classical scrapie. Our results show that CSSA is able to reveal strain-specified PrPSc conformational stabilities of protease-resistant and protease-sensitive PrPSc and that it is a valuable tool for strain typing in natural hosts, such as humans and sheep

    Highly Differentiated, Resting Gn-Specific Memory CD8+ T Cells Persist Years after Infection by Andes Hantavirus

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    In man, infection with South American Andes virus (ANDV) causes hantavirus cardiopulmonary syndrome (HCPS). HCPS due to ANDV is endemic in Southern Chile and much of Argentina and increasing numbers of cases are reported all over South America. A case-fatality rate of about 36% together with the absence of successful antiviral therapies urge the development of a vaccine. Although T-cell responses were shown to be critically involved in immunity to hantaviruses in mouse models, no data are available on the magnitude, specificity and longevity of ANDV-specific memory T-cell responses in patients. Using sets of overlapping peptides in IFN-Îł ELISPOT assays, we herein show in 78 Chilean convalescent patients that Gn-derived epitopes were immunodominant as compared to those from the N- and Gc-proteins. Furthermore, while the relative contribution of the N-specific response significantly declined over time, Gn-specific responses remained readily detectable ex vivo up to 13 years after the acute infection. Tetramer analysis further showed that up to 16.8% of all circulating CD3+CD8+ T cells were specific for the single HLA-B*3501-restricted epitope Gn465–473 years after the acute infection. Remarkably, Gn465–473–specific cells readily secreted IFN-Îł, granzyme B and TNF-α but not IL-2 upon stimulation and showed a ‘revertant’ CD45RA+CD27−CD28−CCR7−CD127− effector memory phenotype, thereby resembling a phenotype seen in other latent virus infections. Most intriguingly, titers of neutralizing antibodies increased over time in 10/17 individuals months to years after the acute infection and independently of whether they were residents of endemic areas or not. Thus, our data suggest intrinsic, latent antigenic stimulation of Gn-specific T-cells. However, it remains a major task for future studies to proof this hypothesis by determination of viral antigen in convalescent patients. Furthermore, it remains to be seen whether Gn-specific T cells are critical for viral control and protective immunity. If so, Gn-derived immunodominant epitopes could be of high value for future ANDV vaccines

    Alzheimer's disease: Clinical practice guideline

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    El Grupo de Trabajo de NeurologĂ­a de la Conducta y Neurociencias Cognitivas de la Sociedad NeurolĂłgica Argentina publicĂł en 2006 la primera GuĂ­a de prĂĄctica clĂ­nica sobre la enfermedad de Alzheimer para su aplicaciĂłn en nuestro medio y, eventualmente, en el resto de los paĂ­ses hispanoparlantes del Cono Sur. La GuĂ­a que hoy publicamos, mediante la revisiĂłn y actualizaciĂłn del estado actual del conocimiento sobre la enfermedad de Alzheimer y su manejo clĂ­nico y neurolĂłgico, provee a los profesionales los estĂĄndares surgidos de la medicina basada en la evidencia para una adecuada implementaciĂłn de las conductas diagnĂłsticas y terapĂ©uticas a su alcance en nuestro medio.In 2006, the Argentine Neurological Society Research Group on Behavioral Neurology and Cognitive Neurosciences published the first Clinical Practice Guideline on Alzheimer's Disease to be consulted in Argentina and eventually in other countries in Latin America. The present Guideline is a review of the state of the art concerning the 2010 knowledge on the management of this disease. It provides physicians with the usual standards provided by evidence based medicine in order to reach the most adequate diagnostic and therapeutic measures at hand in our countries.Fil: Allegri, Ricardo Francisco. Sociedad NeurolĂłgica Argentina; Argentina. FundaciĂłn para la Lucha contra las Enfermedades NeurolĂłgicas de la Infancia. Instituto de Neurociencias - Consejo Nacional de Investigaciones CientĂ­ficas y TĂ©cnicas. Oficina de CoordinaciĂłn Administrativa Ciudad Universitaria. Instituto de Neurociencias; ArgentinaFil: Arizaga, RaĂșl Luciano. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Bavec, Claudia V.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Colli, Liliana P.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Demey, Ignacio. Sociedad NeurolĂłgica Argentina; ArgentinaFil: FernĂĄndez, MarĂ­a C.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Frontera, Silvina A.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Garau, MarĂ­a L.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: JimĂ©nez, Julio J.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Golimstok, Angel. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Kremer, Janus. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Labos, Edith. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Mangone, Carlos Antonio. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Ollari, Juan A.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Rojas, ZenĂłn Galeno. Centro de EducaciĂłn MĂ©dica e Investigaciones ClĂ­nicas "Norberto Quirno"; Argentina. Sociedad NeurolĂłgica Argentina; Argentina. Consejo Nacional de Investigaciones CientĂ­ficas y TĂ©cnicas; ArgentinaFil: Salmini, Omar. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Ure, Jorge A.. Sociedad NeurolĂłgica Argentina; ArgentinaFil: Zuin, Daniel R.. Sociedad NeurolĂłgica Argentina; Argentin
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