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Phagocytosis checkpoints as new targets for cancer immunotherapy

机译:吞噬症检查点作为癌症免疫疗法的新靶标

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摘要

Cancer immunotherapies targeting adaptive immune checkpoints have substantially improved patient outcomes across multiple metastatic and treatment-refractory cancer types. However, emerging studies have demonstrated that innate immune checkpoints, which interfere with the detection and clearance of malignant cells through phagocytosis and suppress innate immune sensing, also have a key role in tumour-mediated immune escape and might, therefore, be potential targets for cancer immunotherapy. Indeed, preclinical studies and early clinical data have established the promise of targeting phagocytosis checkpoints, such as the CD47-signal-regulatory protein alpha (SIRP alpha) axis, either alone or in combination with other cancer therapies. In this Review, we highlight the current understanding of how cancer cells evade the immune system by disrupting phagocytic clearance and the effect of phagocytosis checkpoint blockade on induction of antitumour immune responses. Given the role of innate immune cells in priming adaptive immune responses, an improved understanding of the tumour-intrinsic processes that inhibit essential immune surveillance processes, such as phagocytosis and innate immune sensing, could pave the way for the development of highly effective combination immunotherapy strategies that modulate both innate and adaptive antitumour immune responses.
机译:靶向适应性免疫检查站癌症免疫极大地改善了跨多个转移性和治疗难治性癌症类型的患者的结果。然而,新兴的研究表明,先天免疫检查点,其与检测,并通过吞噬作用,抑制先天免疫传感恶性细胞的清除干扰,也有肿瘤介导的免疫逃逸,并可能在关键的作用,因此,对癌症的潜在目标免疫治疗。事实上,临床前研究和早期临床数据已经建立靶向吞噬检查站,如CD47 - 信号 - 调节蛋白α(SIRP阿尔法)的承诺轴,无论是单独使用或与其它癌症疗法组合。在这次审查中,我们强调的癌细胞是如何通过破坏吞噬清除和吞噬检查站阻断对抗肿瘤免疫应答的诱导作用逃避免疫系统当前的理解。鉴于引发适应性免疫应答,抑制必要的免疫监视过程,如吞噬作用和先天免疫检测肿瘤的内在过程的更好的理解,可以为高度有效结合免疫治疗策略的发展铺平道路先天免疫细胞的作用调节先天性和获得性抗肿瘤免疫反应。

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  • 来源
    《Nature reviews Cancer》 |2019年第10期|共19页
  • 作者单位

    City Hope Comprehens Canc Ctr Beckman Res Inst Dept Immunooncol Duarte CA 91010 USA;

    Univ Texas Southwestern Med Ctr Dallas Dept Radiat Oncol Dallas TX 75390 USA;

    Univ Texas MD Anderson Canc Ctr Dept Neurosurg Houston TX 77030 USA;

    Univ Texas Southwestern Med Ctr Dallas Dept Physiol Dallas TX 75390 USA;

    Univ Texas Southwestern Med Ctr Dallas Dept Pathol Dallas TX USA;

    Stanford Univ Inst Stem Cell Biol &

    Regenerat Med Stanford CA 94305 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 肿瘤学;
  • 关键词

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