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The influence of CD25~+ cells on the generation of immunity to tumour cell lines in mice

机译:CD25〜+细胞对小鼠肿瘤细胞株产生的影响

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CD25~+ regulatory T cells comprise 5-10% of CD4~+ T cells in naive mice and have been shown in several invivo murine models to prevent the induction of autoimmune disease and inflammatory disease. Since T cells, which mediate autoimmunity, can through recognition of self-antigens also "target tumour cells, it was postulated that CD25~+ regulatory cells would also inhibit the generation of immune responses to tumours. Depletion of these cells using CD25-specific monoclonal antibodies has indeed been shown to promote rejection of several ttansplantable murine tumour cell lines including melanoma, leukaemia and colorectal carcinoma Results obtained using these models indicate that in the absence of regulatory cells, CD4~+ T cells mediate tumour immunity, although the precise mechanisms through which these cells result in tumour rejection have not yet been elucidated The target antigens recognized by these CD4~+ T cells have also not yet been identified Immunization of mice with tumour cells in the absence of CD25~+ regulatory cells does, however, induce immunity against a variety of different tumour cell lines indicating that the target antigen(s) are shared amongst tumours of distinct histological origins Since CD25~+ regulatory cells have been identified in humans, the possibility that the cells inhibit immune responses to shared rejection antigens expressed by human tumours is worthy of investigation.
机译:CD25〜+调节性T细胞包含幼稚小鼠中5-10%的CD4〜+ T细胞,已在几种Invivo鼠模型中显示,以防止诱导自身免疫疾病和炎症疾病。由于T细胞,其介导自身免疫,可通过识别也自体抗原“靶肿瘤细胞,据推测,CD25 +调节性细胞也将抑制免疫反应的产生肿瘤。耗尽使用特异性CD25单克隆这些细胞的抗体确实已经显示出促进排斥的几个ttansplantable鼠肿瘤细胞系,包括黑色素瘤,白血病和使用这些模型中获得的结直肠癌结果表明,在不存在调节细胞,CD4 + T细胞介导肿瘤免疫力,虽然确切的机制通过尚未阐明这些细胞导致肿瘤排斥反应尚未阐明这些CD4〜+ T细胞识别的靶抗原,在没有CD25〜+调节细胞的情况下也尚未确定小鼠的小鼠免疫小鼠的免疫,然而,诱导免疫力针对各种不同的肿瘤细胞系,表明靶抗原在Dist的肿瘤中共用由于CD25〜+调节细胞已鉴定在人体中,因此细胞抑制对人肿瘤表达的共用排斥抗原的可能性是值得调查的。

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