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抗 CD20 抗体通过富集表达低水平 CD20 和 CD137L 的肿瘤诱导调节性 B 细胞促进癌症逃逸。

Anti-CD20 antibody promotes cancer escape via enrichment of tumor-evoked regulatory B cells expressing low levels of CD20 and CD137L.

机构信息

Immunotherapeutic Section, National Institute on Aging, Baltimore, MD 21224, USA.

出版信息

Cancer Res. 2013 Apr 1;73(7):2127-38. doi: 10.1158/0008-5472.CAN-12-4184. Epub 2013 Jan 30.

DOI:10.1158/0008-5472.CAN-12-4184
PMID:23365136
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3618504/
Abstract

The possible therapeutic benefits of B-cell depletion in combating tumoral immune escape have been debated. In support of this concept, metastasis of highly aggressive 4T1 breast cancer cells in mice can be abrogated by inactivation of tumor-evoked regulatory B cells (tBreg). Here, we report the unexpected finding that B-cell depletion by CD20 antibody will greatly enhance cancer progression and metastasis. Both murine and human tBregs express low levels of CD20 and, as such, anti-CD20 mostly enriches for these cells. In the 4T1 model of murine breast cancer, this effect of enriching for tBregs suggests that B-cell depletion by anti-CD20 may not be beneficial at all in some cancers. In contrast, we show that in vivo-targeted stimulation of B cells with CXCL13-coupled CpG oligonucleotides (CpG-ODN) can block cancer metastasis by inhibiting CD20(Low) tBregs. Mechanistic investigations suggested that CpG-ODN upregulates low surface levels of 4-1BBL on tBregs to elicit granzyme B-expressing cytolytic CD8(+) T cells, offering some explanative power for the effect. These findings underscore the immunotherapeutic importance of tBreg inactivation as a strategy to enhance cancer therapy by targeting both the regulatory and activating arms of the immune system in vivo.

摘要

B 细胞耗竭在对抗肿瘤免疫逃逸中的可能治疗益处一直存在争议。支持这一概念的是,通过失活肿瘤诱导的调节性 B 细胞(tBreg),可以阻止高度侵袭性 4T1 乳腺癌细胞在小鼠中的转移。在这里,我们报告了一个意外的发现,即通过 CD20 抗体进行 B 细胞耗竭会极大地促进癌症进展和转移。鼠和人 tBregs 表达低水平的 CD20,因此,抗 CD20 主要富集这些细胞。在 4T1 小鼠乳腺癌模型中,这种富集 tBregs 的效应表明,在某些癌症中,抗 CD20 耗竭 B 细胞可能根本没有益处。相比之下,我们发现,体内靶向用 CXCL13 偶联 CpG 寡核苷酸(CpG-ODN)刺激 B 细胞可以通过抑制 CD20(Low) tBregs 来阻断癌症转移。机制研究表明,CpG-ODN 上调 tBregs 上低表面水平的 4-1BBL 以引发表达颗粒酶 B 的细胞毒性 CD8(+) T 细胞,这为这种效应提供了一些解释力。这些发现强调了 tBreg 失活作为一种免疫治疗策略的重要性,通过靶向体内免疫系统的调节和激活臂来增强癌症治疗。

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