972 resultados para Pro-opimélanocortine
Resumo:
Magdeburg, Univ., Med. Fak., Diss., 2011
Resumo:
Haft. 28 (1901-1902)
Resumo:
Haft. 19 (1893)
Resumo:
Haft. 27 (1900-1901)
Resumo:
Haft. 23 (1896-1897)
Resumo:
Haft. 25 (1898-1899)
Resumo:
Haft. 29 (1902-1903)
Resumo:
Haft. 37 (1910-1911)
Resumo:
Haft. 24 (1897-1898)
Resumo:
Haft. 26 (1899-1900)
Resumo:
Haft. 35 (1908-1909)
Resumo:
Haft. 34 (1907-1908)
Resumo:
Haft. 18 (1891-1892)
Resumo:
L’objectiu de la recerca que s’ha dut a terme durant el període 2004-2007 ha estat analitzar les característiques territorials, senyorials i jurisdiccionals del domini format pel comtat de les Muntanyes de Prades i la baronia d’Entença i, a partir d’aquí, aprofundir en un aspecte concret d’aquesta senyoria: l’explotació minera de l’argent durant els segles XIV i XV. En aquest sentit, la recerca s’ha fonamentat en l’estudi de la documentació relacionada amb aquesta qüestió que hi ha dipositada a l’Arxiu Ducal de Medinaceli; la qual, però, s’ha pogut buidar i analitzar a través de la consulta de les còpies microfilmades que se’n conserven al Monestir de Poblet. Com a resultats principals s’ha aconseguit delimitar territorialment el comtat de les Muntanyes de Prades i baronia d’Entença i determinar-ne la titularitat jurisdiccional a mitjan segle XIV. A més, s’han establert els paràmetres que marquen i expliquen l’evolució de la normativa que regulava l’explotació minera de l’argent. I, finalment, s’ha pogut determinar que, segurament, la major part de l’argent produït a mitjan segle XIV es va obtenir a partir de minerals d’argent i argent natiu.
Resumo:
AIMS: Experimental autoimmune myocarditis (EAM) model mirrors important mechanisms of inflammatory dilated cardiomyopathy (iDCM). In EAM, inflammatory CD133(+) progenitors are a major cellular source of cardiac myofibroblasts in the post-inflammatory myocardium. We hypothesized that exogenous delivery of macrophage-colony-stimulating factor (M-CSF) can stimulate macrophage lineage differentiation of inflammatory progenitors and, therefore, prevent their naturally occurring myofibroblast fate in EAM. METHODS AND RESULTS: EAM was induced in wild-type (BALB/c) and nitric oxide synthase 2-deficient (Nos2(-/-)) mice and CD133(+) progenitors were isolated from inflamed hearts. In vitro, M-CSF converted inflammatory CD133(+) progenitors into nitric oxide-producing F4/80(+) macrophages and prevented transforming growth factor-β-mediated myofibroblast differentiation. Importantly, only a subset of heart-infiltrating CD133(+) progenitors expresses macrophage-specific antigen F4/80 in EAM. These CD133(+)/F4/80(hi) cells show impaired myofibrogenic potential compared with CD133(+)/F4/80(-) cells. M-CSF treatment of wild-type mice with EAM at the peak of disease markedly increased CD133(+)/F4/80(hi) cells in the myocardium, and CD133(+) progenitors isolated from M-CSF-treated mice failed to differentiate into myofibroblasts. In contrast, M-CSF was not effective in converting CD133(+) progenitors from inflamed hearts of Nos2(-/-) mice into macrophages, and M-CSF treatment did not result in increased CD133(+)/F4/80(hi) cell population in hearts of Nos2(-/-) mice. Accordingly, M-CSF prevented post-inflammatory fibrosis and left ventricular dysfunction in wild-type but not in Nos2(-/-) mice. CONCLUSION: Active and NOS2-dependent induction of macrophage lineage differentiation abrogates the myofibrogenic potential of heart-infiltrating CD133(+) progenitors. Modulating the in vivo differentiation fate of specific progenitors might become a novel approach for the treatment of inflammatory heart diseases.
