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Multiple pathways to tumor immunity and concomitant autoimmunity.

机译:肿瘤免疫和伴随自身免疫的多种途径。

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摘要

The immune repertoire contains T cells and B cells that can recognize autologous cancer cells. This repertoire is directed against self, and in some cases altered self (mutations). Priming immune responses against self antigens can be difficult. Strategies are presented using altered self to elicit immunity against self in poorly immunogenic tumor models. Mechanisms underlying immunity to self antigens on cancer cells show that the immune system can use diverse strategies for cancer immunity, in both the immunization and the effector phases. CD4+ T cells are typically, but not always, required for immunization. The effector phase of tumor immunity can involve cytotoxic T cells, macrophages with activating Fc receptors, and/or killer domain molecules. This diversity in the effector phase is observed even when immunizing with conserved paralogs. A consequence of tumor immunity is potentially autoimmunity, which may be undesirable. Autoimmunity uses similar mechanisms as tumor immunity, but tumor immunityand autoimmunity can uncouple. These studies open up strategies for active immunization against cancer.
机译:免疫库包含可以识别自体癌细胞的T细胞和B细胞。此曲目是针对自我的,在某些情况下会改变自我(变异)。引发针对自身抗原的免疫反应可能很困难。提出了在免疫原性差的肿瘤模型中使用改变的自身来引发针对自身的免疫力的策略。癌细胞自身抗原免疫的潜在机制表明,免疫系统可以在免疫阶段和效应阶段使用多种策略进行癌症免疫。通常,但并非总是需要免疫接种CD4 + T细胞。肿瘤免疫的效应期可涉及细胞毒性T细胞,具有活化Fc受体的巨噬细胞和/或杀伤域分子。即使在用保守的旁系同源物免疫时,也观察到了效应相的这种多样性。肿瘤免疫的结果是潜在的自身免疫,这可能是不希望的。自身免疫使用与肿瘤免疫类似的机制,但是肿瘤免疫和自身免疫可以分离。这些研究为癌症的主动免疫开辟了策略。

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