38 research outputs found

    Severe Mg-deficiency is not associated with endothelial cell activation in mouse lung

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    Abstract. Several experimental and clinical studies suggest that the lungs are a specific target of Mg-hypomagnesemia, which is a common side effect of cyclosporin A therapy. Due to the possible effect of hypomagnesemia on lung allograft function, the aim of this study was to evaluate endothelial cell (EC) activation and tissue remodelling (apoptosis) in the lungs from mice fed Mg-deficient diets. Immunocytochemical examinations did not reveal any inflammatory process in Mg-deficient mice, infiltration of leukocytes (CD45 + cells), expression of I-A b class II molecules, E-selectin or ICAM-1 on ECs, and apoptotic cells. Quantification of mRNAs for E-selectin, ICAM-1 and VCAM-1, which are the most pertinent adhesins expressed by ECs, and for the cytokines TNFa and IL-2, demonstrated that severe Mg-deficiency does not result in EC activation. The balance between the up-regulation of G-CSF-R and CCL4 genes, and the down-regulation of the OPN gene shown by the cDNA microarray technique might be responsible for the absence of development of an inflammatory response, lung EC activation, and lung remodelling. However, we can hypothesize that severe Mg deficiency results in a latent inflammatory status of the lungs, which might be expressed following immune stresses, like transplantation conditions

    Negative perceptions of aging and decline in walking speed: A self-fulfilling prophecy

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    Introduction Walking speed is a meaningful marker of physical function in the aging population. While it is a primarily physical measure, experimental studies have shown that merely priming older adults with negative stereotypes about aging results in immediate declines in objective walking speed. What is not clear is whether this is a temporary experimental effect or whether negative aging stereotypes have detrimental effects on long term objective health. We sought to explore the association between baseline negative perceptions of aging in the general population and objective walking speed 2 years later. Method 4,803 participations were assessed over 2 waves of The Irish Longitudinal Study on Ageing (TILDA), a prospective, population representative study of adults aged 50+ in the Republic of Ireland. Wave 1 measures – which included the Aging Perceptions Questionnaire, walking speed and all covariates - were taken between 2009 and 2011. Wave 2 measures – which included a second measurement of walking speed and covariates - were collected 2 years later between March and December 2012. Walking speed was measured as the number of seconds to complete the Timed Up-And-Go (TUG) task. Participations with a history of stroke, Parkinson’s disease or an MMSE < 18 were excluded. Results After full adjustment for all covariates (age, gender, level of education, disability, chronic conditions, medications, global cognition and baseline TUG) negative perceptions of aging at baseline were associated with slower TUG speed 2 years later (B=.03, 95% CI = .01 to 05, p< .01). Conclusions Walking speed has previously been considered to be a consequence of physical decline but these results highlight the direct role of psychological state in predicting an objective aging outcome. Negative perceptions about aging are a potentially modifiable risk factor of some elements of physical decline in aging

    Metabolism of lipoproteins in Rodent malaria, Relationship between lipolysis, steatosis and increased biosynthesis of V.L.D.L.

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    The kinetic study of the seric free fatty acids, total lipids and hepatic triacyglycerides had led us to conclude that the biosynthesis of T.A.G.-rich lipoproteins increases during malaria. It seems that the parasite induces a lipolysis of adipose tissue in order to meet its own needs for fatty acids and that the excess of the latter taken by the liver involves an increased synthesis of the V.L.D.L. The cis-vaccenic acid has also been analysed during the evolution of parasitaemia; these variations by themselves cannot explain the extra parasitic hemolysis

    Morphologie et infectivité des gamétocytes de

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    Les auteurs rapportent les changements biomorphologiques subis par les gamétocytes de Plasmodium inui au cours de l’infection naturelle de Macaca fascicularis splénectomisé. L’infection a été suivie jusqu’au 42e jour par des frottis pratiqués par piqûre à l’oreille (P.O.) et sur du sang prélevé au même moment par A. stephensi (P.M.). Les premiers oocystes sont apparus le 8e jour après l’infection chez les moustiques nourris sur le singe parasité 8 jours après la splénectomie, alors que la gamétocytémie n’est pas encore décelable dans les P.O. L’infectivité des gamétocytes a atteint son maximum le 13e jour pour une parasitémie de 152/104. Les premiers sporozoïtes sont apparus le 18e jour à 25°C après le repas infectant. Les sporozoïtes ont été infectants pour un deuxième singe.Quatre types morphologiques (O, I, II et III) de gamétocytes ont été identifiés. Ils correspondent aux types précédemment décrits chez les Plasmodium de rongeur. Le maximum d’infectivité coïncide avec une ascension brutale de la macrogamétocytémie dans les P.M. ; par contre, l’infectivité est très faible lors du pic suivant de macrogamétocytémie qui correspond cependant au maximum de parasitémie (1 318/104 18 jours après la splénectomie).Lorsque l’infectivité est forte, les gamétocytes de type O et I sont plus nombreux dans les P.M. que dans les P.O. pratiqués simultanément.En définitive, le comportement des gamétocytes de P. inui est, pour l’essentiel, très proche de celui des Plasmodium de rongeurs. On notera cependant que l’identification des 4 types morphologiques chez P. inui est plus aisée dans les macrogamétocytes que dans les microgamétocytes. Le contraire avait été observé chez les Plasmodium de rongeurs
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