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靶抗原的组织分布对过继性癌症免疫治疗的结果具有决定性影响。

Tissue distribution of target antigen has a decisive influence on the outcome of adoptive cancer immunotherapy.

作者信息

Meunier Marie-Christine, Roy-Proulx Guillaume, Labrecque Nathalie, Perreault Claude

机构信息

Guy-Bernier Research Center, Maisonneuve-Rosemont Hospital, Montreal, PQ, Canada.

出版信息

Blood. 2003 Jan 15;101(2):766-70. doi: 10.1182/blood-2002-04-1032. Epub 2002 Aug 22.

Abstract

Adoptive transfer of allogeneic T cells has unmatched efficacy to eradicate leukemic cells. We therefore sought to evaluate in kinetic terms interactions between T cells and allogeneic leukemic cells. T cells primed against the model B6(dom1) minor histocompatibility antigen were adoptively transferred in irradiated B10 (B6(dom1)-positive) and congenic B10.H7(b) (B6(dom1)-negative) recipients, some of which were also injected with EL4 leukemia/lymphoma cells (B6(dom1)-positive). A key finding was that the tissue distribution of the target epitope dramatically influenced the outcome of adoptive cancer immunotherapy. Widespread expression of B6(dom1) in B10 recipients induced apoptosis and dysfunction of antigen-specific T cells. Furthermore, in leukemic B10 and B10.H7(b) hosts, a massive accumulation of effector/memory B6(dom1)-specific T cells was detected in the bone marrow, the main site of EL4 cell growth. The accumulation of effector/memory cells in recipient bone marrow was EL4 dependent, and its kinetics was different from that observed in recipient spleen. We conclude that strategies must be devised to prevent apoptosis of adoptively transferred T cells confronted with a high antigen load and that local monitoring of the immune response at the site of tumor growth may be mandatory for a meaningful assessment of the efficacy of adoptive immunotherapy.

摘要

同种异体T细胞的过继转移在根除白血病细胞方面具有无与伦比的疗效。因此,我们试图从动力学角度评估T细胞与同种异体白血病细胞之间的相互作用。用模型B6(dom1)次要组织相容性抗原致敏的T细胞被过继转移到经辐照的B10(B6(dom1)阳性)和同基因B10.H7(b)(B6(dom1)阴性)受体中,其中一些受体还注射了EL4白血病/淋巴瘤细胞(B6(dom1)阳性)。一个关键发现是,靶抗原表位的组织分布显著影响过继性癌症免疫治疗的结果。B10受体中B6(dom1)的广泛表达诱导了抗原特异性T细胞的凋亡和功能障碍。此外,在白血病B10和B10.H7(b)宿主中,在EL4细胞生长的主要部位骨髓中检测到大量效应/记忆B6(dom1)特异性T细胞的积累。效应/记忆细胞在受体骨髓中的积累依赖于EL4,其动力学与在受体脾脏中观察到的不同。我们得出结论,必须设计策略来防止面对高抗原负荷的过继转移T细胞发生凋亡,并且对肿瘤生长部位的免疫反应进行局部监测对于有意义地评估过继性免疫治疗的疗效可能是必不可少的。

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