60 research outputs found

    The association of high-sensitivity c-reactive protein and other biomarkers with cardiovascular disease in patients treated for HIV: a nested case–control study

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    Background: Elevated high-sensitivity C-reactive protein (hsCRP) increases the risk of cardiovascular disease (CVD) in the general population, but its role as a predictive marker in HIV-positive patients remains unclear. Aim of the study was to evaluate whether hsCRP or other biomarkers are independent predictors of CVD risk in HIV-infected patients.Methods: Retrospective, nested case-control study. HIV-positive men and women (35-69 years of age) receiving combination antiretroviral therapy (cART) were included. Cases (n = 35) had a major CVD event. Controls (n = 74) free from CVD events for at least 5 years from starting ART were matched on diabetes and smoking. HsCRP, D-dimer, P-selectin, interleukin-6 (IL-6), tissue plasminogen activator, plasminogen activator inhibitor-1 levels were measured.Results: High hsCRP was associated with CVD risk, independently of traditional cardiovascular risk factors, HIV replication and the type of ART received at the time of sampling (adjusted odds ratio 8.00 [1.23-51.94] comparing >3.3 mg/L with <0.9 mg/L; P = 0.03). Higher IL-6 and P-selectin levels were also independently associated with increased CVD risk, although the association was weaker than for hsCRP. Higher total cholesterol and lower HDL cholesterol increased CVD risk, independent of hsCRP.Conclusion: hsCRP may be a useful additional biomarker to predict CVD risk in HIV-infected patients receiving cART

    The midbody interactome reveals unexpected roles for PP1 phosphatases in cytokinesis

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    Abstract: The midbody is an organelle assembled at the intercellular bridge between the two daughter cells at the end of mitosis. It controls the final separation of the daughter cells and has been involved in cell fate, polarity, tissue organization, and cilium and lumen formation. Here, we report the characterization of the intricate midbody protein-protein interaction network (interactome), which identifies many previously unknown interactions and provides an extremely valuable resource for dissecting the multiple roles of the midbody. Initial analysis of this interactome revealed that PP1ÎČ-MYPT1 phosphatase regulates microtubule dynamics in late cytokinesis and de-phosphorylates the kinesin component MKLP1/KIF23 of the centralspindlin complex. This de-phosphorylation antagonizes Aurora B kinase to modify the functions and interactions of centralspindlin in late cytokinesis. Our findings expand the repertoire of PP1 functions during mitosis and indicate that spatiotemporal changes in the distribution of kinases and counteracting phosphatases finely tune the activity of cytokinesis proteins

    Investigar en Trabajo Social: diferentes experiencias como pasantes de investigaciĂłn

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    El presente trabajo se propone compartir tres experiencias de investigaciĂłn llevadas a cabo por estudiantes (ahora licenciadas) en la Facultad de Trabajo Social de la Universidad Nacional de La Plata, en diferentes proyectos de investigaciĂłn. Dos de las experiencias de pasantĂ­as se enmarcaron en el proyecto de investigaciĂłn “Seguridad, Violencia y Derechos Humanos. Un estudio de las representaciones sociales en jĂłvenes y policĂ­as”1. La otra pasantĂ­a se inserta en el proyecto “Disputas en el espacio pĂșblico: cultura, polĂ­tica y desigualdades socio-urbanas”2. A su vez, dos de nosotras continuamos nuestro proceso de aprendizaje del oficio de investigar a travĂ©s de dos becas CIN en el marco de los proyectos de investigaciĂłn acreditados, mencionados anteriormente. Haremos una breve menciĂłn respecto a esto. Por Ășltimo, analizaremos las experiencias como pasantes de investigaciĂłn a la luz de los aportes de distintos autores/as, haciendo hincapiĂ© principalmente en la comprensiĂłn de las competencias, habilidades y destrezas necesarias para desarrollar la prĂĄctica investigativa.Eje TeĂłrico-metodolĂłgico en Trabajo Social-GT 27: MetodologĂ­a y Trabajo Social.Facultad de Trabajo Socia

    Gorab is a Golgi protein required for structure and duplication of Drosophila centrioles.

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    We demonstrate that a Drosophila Golgi protein, Gorab, is present not only in the trans-Golgi but also in the centriole cartwheel where, complexed to Sas6, it is required for centriole duplication. In addition to centriole defects, flies lacking Gorab are uncoordinated due to defects in sensory cilia, which lose their nine-fold symmetry. We demonstrate the separation of centriole and Golgi functions of Drosophila Gorab in two ways: first, we have created Gorab variants that are unable to localize to trans-Golgi but can still rescue the centriole and cilia defects of gorab null flies; second, we show that expression of C-terminally tagged Gorab disrupts Golgi functions in cytokinesis of male meiosis, a dominant phenotype overcome by mutations preventing Golgi targeting. Our findings suggest that during animal evolution, a Golgi protein has arisen with a second, apparently independent, role in centriole duplication.D.M.G. is grateful for a Wellcome Investigator Award, which supported this work. The study was initiated with support from Cancer Research UK

    The role of the Broad-Complex locus in the expression of genes located at the ecdysone-regulated 3C puff of D. melanogaster.

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    Cytokinesis in Animal Cells

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