首页> 外文会议>Annual Meeting of the Japanese Association for Animal Cell Technology >ESTABLISHMENT AND ANALYSIS OF GERMFREE T CELL RECEPTOR TRANSGENIC MICE
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ESTABLISHMENT AND ANALYSIS OF GERMFREE T CELL RECEPTOR TRANSGENIC MICE

机译:种质型T细胞受体转基因小鼠的建立与分析

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Recent studies have shown that intestinal bacteria affect the intestinal immune system. In order to elucidate the effects of intestinal microflora on T-cell mediated immune responses of the intestine, we established germfree (GF) T cell receptor transgenic (TCR-Tg) mice. GF ovalbumin (OVA)-specific TCR-Tg mice were obtained from conventional (CV) TCR-Tg mice by hysterectomy. Cells from spleen, Peyer's patch (PP) and lamina propria (LP) were isolated from GF TCR-Tg mice, and the ratio of CD4~+ T cellswas assessed by flow cytometry and the production of cytokines, in response to in vitro OVA stimulation, was measured by ELISA. The numbers of PPs were significantly lower in GF TCR-Tg mice compared with CV TCR-Tg mice and the ratios of CD4~+ T cells inPP and LP cells from GF TCR-Tg mice were decreased. When stimulated with OVA, PP cells from GF TCR-Tg mice secreted higher levels of interferon (IFN)--y, interleukin (IL)-5 and IL-6, and LP cells from GF mice secreted higher levels of IFN-y and IL-6 compared with CV mice. These results suggested that although the gut-associated lymphoid tissue is poorly developed in germfree mice, intestinal T cells developing under these conditions possessed an enhanced abih'ty to secrete cylokines in response to antigenic stimulation. Our TCR-Tg system should be an informative system to evaluate the effect of intestinal microflora on antigen-specific T cell responses.
机译:最近的研究表明,肠道细菌影响肠免疫系统。为了阐明肠道微生物对肠炎肠道介导的免疫应答的影响,我们建立了Germfree(GF)T细胞受体转基因(TCR-TG)小鼠。 GF ovalbumin(OVA)特异性TCR-TG小鼠通过子宫切除术获得从常规(CV)TCR-TG小鼠获得。从GF TCR-TG小鼠中分离来自脾脏,Peyer的贴剂(PP)和层丙蛋白(LP)的细胞,以及通过流式细胞术评估的CD4〜+ T Cellswas的比例和细胞因子的产生,响应于体外卵子刺激,由ELISA测量。与CV TCR-TG小鼠相比,GF TCR-TG小鼠中PPS的数量显着降低,CD4〜+ T细胞INPP和来自GF TCR-TG小鼠的LP细胞的比例的比例较低。当用OVA刺激时,来自GF TCR-TG小鼠的PP细胞分泌更高水平的干扰素(IFN) - Y,白细胞介素(IL)-5和IL-6,以及来自GF小鼠的LP细胞分泌更高水平的IFN-Y和IL-6与CV小鼠相比。这些结果表明,虽然肠道相关的淋巴组织在种质小鼠中发育不良,但在这些条件下发育的肠T细胞具有增强的ABIH,以响应抗原刺激分泌圆锥圆锥。我们的TCR-TG系统应该是一种信息化系统,以评估肠道微生物对抗原特异性T细胞反应的影响。

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