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首页> 外文期刊>International Journal for Parasitology >Dynamics of hepatic stellate cells, collagen types I and III synthesis and gene expression of selected cytokines during hepatic fibrogenesis following Mesocestoides vogae (Cestoda) infection in mice.
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Dynamics of hepatic stellate cells, collagen types I and III synthesis and gene expression of selected cytokines during hepatic fibrogenesis following Mesocestoides vogae (Cestoda) infection in mice.

机译:小鼠中鼻咽癌(Mesocestoides vogae(Cestoda))感染后肝纤维化过程中,肝星状细胞,I型和III型胶原合成以及所选细胞因子基因表达的动态。

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In the present study, the relationship between progression of Mesocestoides vogae infection in the liver of mice, the accumulation rate of collagen types I and III, gene expression of fibrogenic factors and cytokines was examined within 6weeks p.i. Due to asexual multiplication, the total number of larvae in the liver increased considerably and 63.4% were found in collagen capsules on day 42 p.i. Intense staining for both collagens was recorded in the activated hepatic stellate cells (HSCs) throughout the period of this study in the inflammatory lesions. With progressing infection, cellular expression of both collagens was confined to the flat cells, myofibroblasts, which were scattered among collagen fibres in parenchymal lesions and capsules. Collagen-positive areas mirrored immunostaining of alpha-smooth muscle actin (alpha-SMA) in HSCs and myofibroblasts. Gene expression of both collagens increased rapidly within 14days p.i. and their expression pattern resembled that for pro-fibrotic cytokine transforming growth factor (TGF)-beta1 and alpha-SMA protein. IL-10 cytokine expression was up-regulated following day 14 p.i. and that of IL-13 was up-regulated early p.i., then transcription elevated gradually mirroring the activity of other pro-fibrotic markers. In contrast, transcription activity of TNF-alpha and IFN-gamma was elevated shortly after infection, followed by the partial down-regulation of gene expression, indicating the lack of larval killing, enhanced granulomatous inflammation and the perpetuation of hepatic fibrosis. Histomorphometric analysis of the parenchymal fibrous lesions, surface areas of larvae surrounded with the inflammatory infiltrates and surface areas of developing or mature larva-containing granulomas, correlated with the proportion of free and encapsulated larvae, immunostaining and gene expression patterns of collagens and pro-fibrotic markers. At a later stage of infection (day 28 p.i. onwards) collagen I-positive areas occupied a greater surface area and formed mature larval capsules and scars in the liver. In contrast, collagen III was less abundant and was localised mainly in the fibrous lesions in damaged parenchyma, suggesting their specific up-regulation as the part of host-protecting and tissue-healing responses.
机译:在本研究中,在小鼠腹腔注射后6周内检查了小鼠肝脏中的小肠鞭毛虫感染进展,I型和III型胶原蛋白的蓄积率,纤维化因子的基因表达和细胞因子之间的关系。由于无性繁殖,肝脏中幼虫的总数显着增加,在第42天的第24天,胶原蛋白胶囊中发现了63.4%。在整个研究过程中,在炎性病变中,活化的肝星状细胞(HSC)中均记录了两种胶原蛋白的强烈染色。随着感染的进行,两种胶原蛋白的细胞表达都局限于扁平细胞,成肌纤维细胞,它们散布在实质性病变和囊膜的胶原蛋白纤维之间。胶原蛋白阳性区域反映了HSC和成肌纤维细胞中α平滑肌肌动蛋白(α-SMA)的免疫染色。两种胶原蛋白的基因表达在p.i的14天内迅速增加。其表达模式类似于促纤维化细胞因子转化生长因子(TGF)-beta1和α-SMA蛋白。第14天p.i后,IL-10细胞因子的表达上调。 IL-13的表达在p.i.早期被上调,然后转录逐渐升高,反映了其他促纤维化标记物的活性。相反,感染后不久,TNF-α和IFN-γ的转录活性升高,随后基因表达部分下调,表明缺乏幼虫杀伤,肉芽肿性炎症增强和肝纤维化永存。组织形态计量学分析的实质性纤维病变,幼虫的表面积被炎性浸润包围和发育或成熟的含有幼虫的肉芽肿的表面积,与游离和封装的幼虫的比例,胶原的免疫染色和基因表达模式和促纤维化相关标记。在感染的后期(下午28天以后),胶原蛋白I阳性区域占据了较大的表面积,并在肝脏中形成了成熟的幼虫囊和疤痕。相比之下,III型胶原蛋白含量较低,主要分布在受损的实质中的纤维性病变中,表明它们的特定上调是宿主保护和组织修复反应的一部分。

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