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首页> 外文期刊>anatomical record >Factors influencing fetal macrophage development .3. Immunocytochemical localization of cytokines and time-resolved expression of differentiation markers in organ-cultured rat lungs
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Factors influencing fetal macrophage development .3. Immunocytochemical localization of cytokines and time-resolved expression of differentiation markers in organ-cultured rat lungs

机译:Factors influencing fetal macrophage development .3. Immunocytochemical localization of cytokines and time-resolved expression of differentiation markers in organ-cultured rat lungs

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abstract_textpBackground: Exogenous TNF alpha, IL-1 beta, M-CSF, and GM-CSF all stimulate growth of macrophages arising in explanted fetal rat lungs. The present study examines the intrinsic availability of these factors in intact and organ-cultured lungs and utilizes expression of cytokines and marker proteins to explore the differentiation pathway followed by phagocytes in vitro./ppMethods: Factors and markers were localized immunocytochemically in paraffin sections of 14- and 15-day fetal rat lungs and lungs organ-cultured up to 7 days on serum-containing medium solidified with agar. Western analyses for the cytokines were performed on lysates of whole 15-day lungs, and in situ hybridization of M-CSF receptor mRNA was carried out in sections of 14 + 2 day cultured lung./ppResults: IL-1 beta, M-CSF, and GM-CSF were demonstrated in the stroma of intact and cultured lungs by immunostaining, results confirmed by Western blotting. TNF alpha appeared to be absent. A few precursors (angular cells) expressed the macrophage lineage marker RM-1 as early as day 14, and immunostaining became stronger and more widespread as the population matured and expanded in cultures. The OX-6 antibody to Ia antigen first reacted with macrophages in 14 + 1 day explants, and within a week 50 of cells were positive. M-CSF and mRNA for its receptor were present at 14 + 2 days, as was PDGF, which had been demonstrated in the stroma and epithelium prior to explantation. Definite reactivity for IL-1 beta and GM-CSF followed at 14 + 4 and 14 + 5 days./ppConclusions: M-CSF, GM-CSF, and IL-1 beta, but not TNF alpha, are available to replicating angular cells before and during their conversion to phagocytes. Fetal lungs thus qualify as a hematopoietic tissue supportive of macrophages. The path of differentiation pursued in organ cultures involves early expression of structural elements (RM-1, Ia antigen) followed by synthesis of cytokines of the TNF alpha cascade. Immunostaining for both RM-1 and OX-6 suggests that fetal lung macrophages share a common heritage with antigen-presenting pulmonary dendritic cells. (C) 1997 Wiley-Liss, Inc./p/abstract_text
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