16 research outputs found

    ROGERS (Rebecca). A Frenchwoman’s Imperial Story. Madame Luce in Nineteenth-Century Algeria

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    La vie d’une institutrice provinciale apparemment sans histoire, arrivée à Alger en 1832 et fondatrice en 1845 de la première école pour jeunes filles musulmanes de la ville, nous apprend-elle quelque chose de la société coloniale d’alors ? C’est ce défi que relève l’historienne Rebecca Rogers dans le très beau livre qu’elle consacre à Eugénie Allix Luce (1804-1882). Inconnue aujourd’hui, cette dernière bénéficia d’une certaine notoriété de son temps et ce, bien au-delà des frontières de l’em..

    ROGERS (Rebecca). A Frenchwoman’s Imperial Story. Madame Luce in Nineteenth-Century Algeria

    Get PDF
    La vie d’une institutrice provinciale apparemment sans histoire, arrivée à Alger en 1832 et fondatrice en 1845 de la première école pour jeunes filles musulmanes de la ville, nous apprend-elle quelque chose de la société coloniale d’alors ? C’est ce défi que relève l’historienne Rebecca Rogers dans le très beau livre qu’elle consacre à Eugénie Allix Luce (1804-1882). Inconnue aujourd’hui, cette dernière bénéficia d’une certaine notoriété de son temps et ce, bien au-delà des frontières de l’em..

    Resveratrol Increases Glucose Induced GLP-1 Secretion in Mice: A Mechanism which Contributes to the Glycemic Control

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    Resveratrol (RSV) is a potent anti-diabetic agent when used at high doses. However, the direct targets primarily responsible for the beneficial actions of RSV remain unclear. We used a formulation that increases oral bioavailability to assess the mechanisms involved in the glucoregulatory action of RSV in high-fat diet (HFD)-fed diabetic wild type mice. Administration of RSV for 5 weeks reduced the development of glucose intolerance, and increased portal vein concentrations of both Glucagon-like peptid-1 (GLP-1) and insulin, and intestinal content of active GLP-1. This was associated with increased levels of colonic proglucagon mRNA transcripts. RSV-mediated glucoregulation required a functional GLP-1 receptor (Glp1r) as neither glucose nor insulin levels were modulated in Glp1r-/- mice. Conversely, levels of active GLP-1 and control of glycemia were further improved when the Dipeptidyl peptidase-4 (DPP-4) inhibitor sitagliptin was co-administered with RSV. In addition, RSV treatment modified gut microbiota and decreased the inflammatory status of mice. Our data suggest that RSV exerts its actions in part through modulation of the enteroendocrine axis in vivo

    The glucose control by RSV is blunted in high fat diet-fed Glp1r<sup>−/−</sup> mice.

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    <p><b>A)</b> Glycemic profiles (mg/dL) of high fat diet-fed Glp1r<sup>−/−</sup> mice treated with vehicle (triangles) or RSV (squares) for five weeks and <b>B)</b> an index of area under the curve glucose (AUC); <b>C)</b> proglucagon mRNA levels (Relative expression level REL) of high fat diet-fed mice treated with vehicle (open bars) and RSV (closed bars) for five weeks. <b>D)</b> Glycemic profiles (mg/dL) of high fat diet-fed wild type mice (high fat diet-fed mice treated with vehicule (white triangles) or RSV (white squares)) and Glp1r<sup>−/−</sup> mice (high fat diet-fed mice treated with vehicule (black triangles) or RSV (black squares)) after five weeks of treatment and <b>E)</b> an index of area under the curve glucose (AUC). Data are presented as mean ± S.E.M, n = 8 mice per group.</p

    Co-administration of the dipeptidyl peptidase-4 inhibitor sitaglipin and RSV further improves glucose tolerance in high fat diet-fed diabetic mice.

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    <p><b>A)</b> Glycemic profiles (mg/dL) of high fat diet-fed diabetic mice treated with RSV (squares), or RSV plus sitagliptin (triangles) for five weeks; <b>B)</b> portal vein active GLP-1 concentrations (pM) and <b>C)</b> proglucagon mRNA levels (Relative Expression Level REL) of high at diet-fed mice treated with RSV (closed bars) and sitagliptin plus RSV (spotted bars) for five weeks. Data are presented as mean ±S.E.M, n = 8 mice per group, * and *** statistically different between groups when p<0.05 and p<0.001, respectively, as analyzed by the Student's T test.</p

    RSV decreases the inflammatory status in high fat-fed diabetic mice.

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    <p>IL-10 mRNA levels (Relative Expression Level, REL) <b>(A)</b> and IL-10 protein concentration (µg/g) <b>(B)</b> in colon; IL-10 mRNA in liver <b>(C)</b> and muscle <b>(D)</b>, TGF-β mRNA in colon <b>(E)</b>, liver <b>(F)</b>, muscle <b>(G)</b>, and TNF-α mRNA in colon <b>(H)</b>, liver <b>(I)</b>, muscle <b>(J)</b> of normal chow (stripe bars), high fat diet-fed mice treated with vehicle (open bars) or RSV (closed bars) for five weeks. Data are presented as mean ± S.E.M, n = 8 mice per group (in fed state) *, ** and *** statistically different between groups when p<0.05, p<0.01 and p<0.001, respectively, as analyzed by the Student's T test (<a href="http://www.plosone.org/article/info:doi/10.1371/journal.pone.0020700#pone-0020700-g006" target="_blank">Fig. 6B</a>) and one-way ANOVA followed by Tukey test. (<a href="http://www.plosone.org/article/info:doi/10.1371/journal.pone.0020700#pone-0020700-g006" target="_blank">Fig. 6A, C, D, E, F, G, H, I, J</a>).</p
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