癌症特异性T细胞“看到”了什么?

Discovery immunology Pub Date : 2022-12-06 eCollection Date: 2023-01-01 DOI:10.1093/discim/kyac011
Sabaria Shah, Abdullah Al-Omari, Katherine W Cook, Samantha J Paston, Lindy G Durrant, Victoria A Brentville
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引用次数: 0

摘要

免疫系统和癌症之间复杂的细胞相互作用可以影响肿瘤的发展、生长和进展。T细胞在这些相互作用中发挥着关键作用,然而,T细胞面临的挑战是识别肿瘤抗原,同时最大限度地减少与健康组织相关抗原的交叉反应。一些肿瘤细胞,包括与病毒感染相关的肿瘤细胞,具有明确的肿瘤特异性抗原,可以被T细胞靶向。高突变负荷可导致突变新抗原数量增加,这允许产生非常特异的免疫反应,但也允许发展逃逸变异。其他癌症适应症和突变负担低的适应症不太容易与正常组织区分开来。最近的研究表明,肿瘤细胞生物学中与癌症相关的改变,包括翻译后修饰(PTM)模式的改变,也可能导致T细胞直接识别的新抗原。PTM衍生的抗原提供肿瘤特异性T细胞反应,既逃避了中心耐受,又避免了个体化治疗的必要性。PTM特异性CD4 T细胞反应在小鼠模型中显示了肿瘤治疗,并强调了CD4 T淋巴细胞和CD8 T细胞在逆转免疫抑制肿瘤微环境中的重要性。了解哪些癌症特异性抗原可以被T细胞识别,以及免疫耐受和肿瘤微环境如何形成对癌症的免疫反应,对于癌症疗法的未来发展至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
What do cancer-specific T cells 'see'?

Complex cellular interactions between the immune system and cancer can impact tumour development, growth, and progression. T cells play a key role in these interactions; however, the challenge for T cells is to recognize tumour antigens whilst minimizing cross-reactivity with antigens associated with healthy tissue. Some tumour cells, including those associated with viral infections, have clear, tumour-specific antigens that can be targeted by T cells. A high mutational burden can lead to increased numbers of mutational neoantigens that allow very specific immune responses to be generated but also allow escape variants to develop. Other cancer indications and those with low mutational burden are less easily distinguished from normal tissue. Recent studies have suggested that cancer-associated alterations in tumour cell biology including changes in post-translational modification (PTM) patterns may also lead to novel antigens that can be directly recognized by T cells. The PTM-derived antigens provide tumour-specific T-cell responses that both escape central tolerance and avoid the necessity for individualized therapies. PTM-specific CD4 T-cell responses have shown tumour therapy in murine models and highlight the importance of CD4 T cells as well as CD8 T cells in reversing the immunosuppressive tumour microenvironment. Understanding which cancer-specific antigens can be recognized by T cells and the way that immune tolerance and the tumour microenvironment shape immune responses to cancer is vital for the future development of cancer therapies.

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