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p53对抗肿瘤免疫的影响(综述)

Influence of p53 on anti-tumor immunity (review).

作者信息

Bueter Marco, Gasser Martin, Lebedeva Tatiana, Benichou Gilles, Waaga-Gasser Ana Maria

机构信息

Department of Surgery I, Molecular Oncology and Immunology, University of Wuerzburg, D-97080 Wuerzburg, Germany.

出版信息

Int J Oncol. 2006 Feb;28(2):519-25.

Abstract

Self-tolerance and tumor-induced peripheral tolerance may be responsible for the limitations of the immune system in controlling tumor growth in cancer patients. It is known, that self-proteins are continuously processed and presented by antigen presenting cells. During development, auto-reactive T cells encountering self peptide/self-MHC complexes are being eliminated in the thymus. This process called 'negative selection' results in the removal of nascent auto-reactive T cells thus preventing an autoimmune attack of our own tissues. Many self-peptides (e.g. parts of p53), despite their high affinity for self-MHC, remain cryptic in the thymus and do not mediate cell deletion. Under conditions that favor up-regulation of cryptic self-determinants, one or more of these subsets of the 'protected' T cell repertoires, can be stimulated by these self-determinants, leading to induction of autoreactivity. The latter could eventually result in auto-immunity under permissive conditions governed by MHC and non-MHC genes. Thus, considering tumor tissue a 'modified self-tissue', this process that may have evolved to prevent excessive purge of the T cell repertoire, providing the potential for the development of autoimmune responses and therefore for anti-cancer therapy in adults.

摘要

自身耐受性和肿瘤诱导的外周耐受性可能是癌症患者免疫系统在控制肿瘤生长方面存在局限性的原因。众所周知,抗原呈递细胞会持续处理并呈递自身蛋白质。在发育过程中,遇到自身肽/自身MHC复合物的自身反应性T细胞会在胸腺中被清除。这个被称为“阴性选择”的过程会导致新生的自身反应性T细胞被清除,从而防止对自身组织的自身免疫攻击。许多自身肽(例如p53的部分片段),尽管它们与自身MHC具有高亲和力,但在胸腺中仍处于隐匿状态,不会介导细胞清除。在有利于隐匿性自身决定簇上调的条件下,这些“受保护”的T细胞库的一个或多个亚群可以被这些自身决定簇刺激,从而导致自身反应性的诱导。在由MHC和非MHC基因控制的允许条件下,后者最终可能导致自身免疫。因此,将肿瘤组织视为“修饰的自身组织”,这个可能已经进化以防止T细胞库过度清除的过程,为自身免疫反应的发展提供了可能性,因此也为成人的抗癌治疗提供了可能性。

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