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过继转移的体外扩增γδ T 细胞在乳腺癌临床前小鼠模型中介导体内抗肿瘤活性。

Adoptively transferred ex vivo expanded gammadelta-T cells mediate in vivo antitumor activity in preclinical mouse models of breast cancer.

机构信息

Department of Medicine, Division of Hematology and Oncology, University of Alabama at Birmingham, SHEL 571, 1825 University Boulevard, Birmingham, AL 35294, USA.

出版信息

Breast Cancer Res Treat. 2010 Jul;122(1):135-44. doi: 10.1007/s10549-009-0527-6. Epub 2009 Sep 18.

Abstract

In contrast to antigen-specific alphabeta-T cells (adaptive immune system), gammadelta-T cells can recognize and lyse malignantly transformed cells almost immediately upon encounter in a manner that does not require the recognition of tumor-specific antigens (innate immune system). Given the well-documented capacity of gammadelta-T cells to innately kill a variety of malignant cells, efforts are now actively underway to exploit the antitumor properties of gammadelta-T cells for clinical purposes. Here, we present for the first time preclinical in vivo mouse models of gammadelta-T cell-based immunotherapy directed against breast cancer. These studies were explicitly designed to approximate clinical situations in which adoptively transferred gammadelta-T cells would be employed therapeutically against breast cancer. Using radioisotope-labeled gammadelta-T cells, we first show that adoptively transferred gammadelta-T cells localize to breast tumors in a mouse model (4T1 mammary adenocarcinoma) of human breast cancer. Moreover, by using an antibody directed against the gammadelta-T cell receptor (TCR), we determined that localization of adoptively transferred gammadelta-T cells to tumor is a TCR-dependant process. Additionally, biodistribution studies revealed that adoptively transferred gammadelta-T cells traffic differently in tumor-bearing mice compared to healthy mice with fewer gammadelta-T cells localizing into the spleens of tumor-bearing mice. Finally, in both syngeneic (4T1) and xenogeneic (2Lmp) models of breast cancer, we demonstrate that adoptively transferred gammadelta-T cells are both effective against breast cancer and are otherwise well-tolerated by treated animals. These findings provide a strong preclinical rationale for using ex vivo expanded adoptively transferred gammadelta-T cells as a form of cell-based immunotherapy for the treatment of breast cancer. Additionally, these studies establish that clinically applicable methods for radiolabeling gammadelta-T cells allows for the tracking of adoptively transferred gammadelta-T cells in tumor-bearing hosts.

摘要

与抗原特异性的 αβ-T 细胞(适应性免疫系统)相反,γδ-T 细胞在遇到恶性转化细胞时几乎可以立即识别并裂解它们,而无需识别肿瘤特异性抗原(先天免疫系统)。鉴于 γδ-T 细胞具有先天杀死多种恶性细胞的能力,现在正在积极努力利用 γδ-T 细胞的抗肿瘤特性用于临床目的。在这里,我们首次提出了针对乳腺癌的基于 γδ-T 细胞的免疫治疗的临床前体内小鼠模型。这些研究专门设计用于模拟临床上采用过继转移 γδ-T 细胞治疗乳腺癌的情况。使用放射性同位素标记的 γδ-T 细胞,我们首先证明过继转移的 γδ-T 细胞在乳腺癌的小鼠模型(4T1 乳腺腺癌)中定位于乳腺肿瘤。此外,通过使用针对 γδ-T 细胞受体(TCR)的抗体,我们确定了过继转移的 γδ-T 细胞定位于肿瘤是 TCR 依赖性过程。此外,生物分布研究表明,与健康小鼠相比,携带肿瘤的小鼠中过继转移的 γδ-T 细胞的分布方式不同,携带肿瘤的小鼠中更少的 γδ-T 细胞定位于脾脏。最后,在同源(4T1)和异种(2Lmp)乳腺癌模型中,我们证明过继转移的 γδ-T 细胞对乳腺癌均有效,并且治疗动物的耐受性良好。这些发现为使用体外扩增的过继转移 γδ-T 细胞作为一种细胞免疫疗法治疗乳腺癌提供了强有力的临床前依据。此外,这些研究确立了用于放射性标记 γδ-T 细胞的临床适用方法,可用于跟踪肿瘤宿主中过继转移的 γδ-T 细胞。

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