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Immune selection in neoplasia: towards a microevolutionary model of cancer development

机译:瘤形成中的免疫选择:朝着癌症发展的微进化模型发展

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摘要

The dual properties of genetic instability and clonal expansion allow the development of a tumour to occur in a microevolutionary fashion. A broad range of pressures are exerted upon a tumour during neoplastic development. Such pressures are responsible for the selection of adaptations which provide a growth or survival advantage to the tumour. The nature of such selective pressures is implied in the phenotype of tumours that have undergone selection. We have reviewed a range of immunologically relevant adaptations that are frequently exhibited by common tumours. Many of these have the potential to function as mechanisms of immune response evasion by the tumour. Thus, such adaptations provide evidence for both the existence of immune surveillance, and the concept of immune selection in neoplastic development. This line of reasoning is supported by experimental evidence from murine models of immune involvement in neoplastic development. The process of immune selection has serious implications for the development of clinical immunotherapeutic strategies and our understanding of current in vivo models of tumour immunotherapy. © 2000 Cancer Research Campaign
机译:遗传不稳定性和克隆扩增的双重性质允许肿瘤以微进化方式发生。在肿瘤形成过程中,广泛的压力施加在肿瘤上。这种压力负责选择适应性,从而为肿瘤提供生长或生存优势。这种选择压力的性质暗示了已经进行选择的肿瘤的表型。我们已经审查了常见肿瘤经常表现出的一系列与免疫学相关的适应性变化。其中许多具有作为肿瘤逃避免疫应答机制的潜力。因此,这种适应为免疫监控的存在以及肿瘤发展中免疫选择的概念提供了证据。来自肿瘤发展中免疫参与的鼠模型的实验证据支持了这一推理。免疫选择的过程对临床免疫治疗策略的发展以及我们对当前肿瘤免疫疗法的体内模型的理解具有重要意义。 ©2000癌症研究运动

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