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解码癌症中的T细胞衰老:是否需要重新审视?

Decoding T cell senescence in cancer: Is revisiting required?

作者信息

Magkouta Sophia, Markaki Efrosyni, Evangelou Konstantinos, Petty Russell, Verginis Panayotis, Gorgoulis Vassilis

机构信息

Molecular Carcinogenesis Group, Department of Histology and Embryology, Medical School, National and Kapodistrian University of Athens, Athens 11527, Greece; Marianthi Simou and G.P. Livanos Labs, 1st Department of Critical Care and Pulmonary Services, School of Medicine, National & Kapodistrian University of Athens, "Evangelismos" Hospital, Athens 10676, Greece; Ninewells Hospital and Medical School, University of Dundee, Dundee DD19SY, UK.

Laboratory of Immune Regulation and Tolerance, Division of Basic Sciences, University of Crete Medical School, Heraklion 70013, Greece.

出版信息

Semin Cancer Biol. 2025 Jan;108:33-47. doi: 10.1016/j.semcancer.2024.11.003. Epub 2024 Nov 29.

Abstract

Senescence is an inherent cellular mechanism triggered as a response to stressful insults. It associates with several aspects of cancer progression and therapy. Senescent cells constitute a highly heterogeneous cellular population and their identification can be very challenging. In fact, the term "senescence" has been often misused. This is also true in the case of immune cells. While several studies indicate the presence of senescent-like features (mainly in T cells), senescent immune cells are poorly described. Under this prism, we herein review the current literature on what has been characterized as T cell senescence and provide insights on how to accurately discriminate senescent cells against exhausted or anergic ones. We also summarize the major metabolic and epigenetic modifications associated with T cell senescence and underline the role of senescent T cells in the tumor microenvironment (TME). Moreover, we discuss how these cells associate with standard clinical therapeutic interventions and how they impact their efficacy. Finally, we underline the importance of precise identification and thorough characterization of "truly" senescent T cells in order to design successful therapeutic manipulations that would delay cancer incidence and maximize efficacy of immunotherapy.

摘要

衰老 是一种内在的细胞机制,作为对压力性损伤的反应而被触发。它与癌症进展和治疗的多个方面相关。衰老细胞构成了一个高度异质性的细胞群体,对它们的识别可能非常具有挑战性。事实上,“衰老”一词经常被误用。免疫细胞的情况也是如此。虽然多项研究表明存在衰老样特征(主要在T细胞中),但衰老免疫细胞的描述却很少。在此背景下,我们在此回顾了关于被称为T细胞衰老的当前文献,并就如何准确区分衰老细胞与耗竭或无反应细胞提供见解。我们还总结了与T细胞衰老相关的主要代谢和表观遗传修饰,并强调了衰老T细胞在肿瘤微环境(TME)中的作用。此外,我们讨论了这些细胞如何与标准临床治疗干预相关联以及它们如何影响其疗效。最后,我们强调精确识别和全面表征“真正”衰老T细胞的重要性,以便设计出能够延缓癌症发生并最大化免疫治疗疗效的成功治疗策略。

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