调节性T细胞与肿瘤免疫中的先天免疫调节。

Springer seminars in immunopathology Pub Date : 2006-08-01 Epub Date: 2006-07-13 DOI:10.1007/s00281-006-0022-7
Rong-Fu Wang
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引用次数: 7

摘要

先天免疫和适应性免疫在免疫监视和肿瘤破坏中发挥着重要作用。然而,越来越多的证据表明,肿瘤浸润性免疫细胞可能具有双重功能:抑制或促进肿瘤的生长和进展。虽然调节性T (Treg)细胞通过抑制宿主对自身或非自身抗原的免疫反应诱导免疫耐受,从而在预防自身免疫性疾病中发挥关键作用,但它们可能抑制抗肿瘤免疫并促进肿瘤生长。最近的研究表明,Treg细胞的比例升高存在于各种类型的癌症中,并抑制抗肿瘤免疫。此外,肿瘤特异性Treg细胞只有在暴露于肿瘤细胞呈递的抗原时才能抑制免疫反应。因此,肿瘤部位的Treg细胞对针对癌症的免疫治疗有不利影响。本文将讨论先天性免疫、Treg细胞及其通过toll样受体(TLR)信号调控的最新进展。一般认为,tlr介导的对入侵病原体特异性结构的识别通过树突状细胞启动先天和适应性免疫反应。新的证据表明,TLR信号可能直接调节Treg细胞的抑制功能。将TLR信号与Treg细胞的功能控制联系起来,为操纵TLR信号以控制抗癌的先天和适应性免疫提供了有趣的机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Regulatory T cells and innate immune regulation in tumor immunity.

Innate and adaptive immunity play important roles in immunosurveillance and tumor destruction. However, increasing evidence suggests that tumor-infiltrating immune cells may have a dual function: inhibiting or promoting tumor growth and progression. Although regulatory T (Treg) cells induce immune tolerance by suppressing host immune responses against self- or nonself-antigens, thus playing critical roles in preventing autoimmune diseases, they might inhibit antitumor immunity and promote tumor growth. Recent studies demonstrate that elevated proportions of Treg cells are present in various types of cancers and suppress antitumor immunity. Furthermore, tumor-specific Treg cells can inhibit immune responses only when they are exposed to antigens presented by tumor cells. Therefore, Treg cells at tumor sites have detrimental effects on immunotherapy directed to cancer. This review will discuss recent progress in innate immunity, Treg cells, and their regulation through Toll-like receptor (TLR) signaling. It was generally thought that TLR-mediated recognition of specific structures of invading pathogens initiate innate and adaptive immune responses through dendritic cells. New evidence suggests that TLR signaling may directly regulate the suppressive function of Treg cells. Linking TLR signaling to the functional control of Treg cells opens intriguing opportunities to manipulate TLR signaling to control both innate and adaptive immunity against cancer.

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