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休眠抗肿瘤免疫的重新激活——治疗性免疫检查点调节的临床视角

Reactivation of dormant anti-tumor immunity - a clinical perspective of therapeutic immune checkpoint modulation.

作者信息

Greil Richard, Hutterer Evelyn, Hartmann Tanja Nicole, Pleyer Lisa

机构信息

Third Medical Department with Hematology, Medical Oncology, Hemostaseology, Infectious Disease and Rheumatology, Oncologic Center, Paracelsus Medical University Salzburg, Müllner Hauptstraße 48, A-5020, Salzburg, Austria.

Salzburg Cancer Research Institute (SCRI) - Laboratory for Immunological and Molecular Cancer Research (LIMCR), Salzburg, Austria.

出版信息

Cell Commun Signal. 2017 Jan 19;15(1):5. doi: 10.1186/s12964-016-0155-9.

Abstract

In favor of their outgrowth, cancer cells must resist immune surveillance and edit the immune response. Cancer immunoediting is characterized by fundamental changes in the cellular composition and the inflammatory cytokine profiles in the microenvironment of the primary tumor and metastatic niches, with an ever increasing complexity of interactions between tumor cells and the immune system. Recent data suggest that genetic instability and immunoediting are not necessarily disparate processes. Increasing mutational load may be associated with multiple neoepitopes expressed by the tumor cells and thus increased chances for the immune system to recognize and combat these cells. At the same time the immune system is more and more suppressed and exhausted by this process. Consequently, immune checkpoint modulation may have the potential to be most successful in genetically highly altered and usually extremely unfavorable types of cancer. Moreover, the fact that epitopes recognized by the immune system are preferentially encoded by passenger gene mutations opens windows of synergy in targeting cancer-specific signaling pathways by small molecules simultaneously with antibodies modifying T-cell activation or exhaustion.This review covers some aspects of the current understanding of the immunological basis necessary to understand the rapidly developing therapeutic endeavours in cancer treatment, the clinical achievements made, and raises some burning questions for translational research in this field.

摘要

为了实现增殖,癌细胞必须抵抗免疫监视并编辑免疫反应。癌症免疫编辑的特征在于原发性肿瘤和转移微环境中细胞组成和炎性细胞因子谱的根本变化,肿瘤细胞与免疫系统之间的相互作用日益复杂。最近的数据表明,基因不稳定和免疫编辑不一定是不同的过程。增加的突变负荷可能与肿瘤细胞表达的多个新表位相关,从而增加免疫系统识别和对抗这些细胞的机会。同时,免疫系统在此过程中越来越受到抑制和耗竭。因此,免疫检查点调节可能在基因高度改变且通常极为不利的癌症类型中最有可能取得成功。此外,免疫系统识别的表位优先由过客基因突变编码这一事实,为小分子与修饰T细胞激活或耗竭的抗体同时靶向癌症特异性信号通路开辟了协同作用的窗口。本综述涵盖了当前对理解癌症治疗中快速发展的治疗努力所需的免疫学基础的一些认识、所取得的临床成就,并提出了该领域转化研究中一些亟待解决的问题。

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