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CD40配体在RNA脉冲树突状细胞免疫疗法中对于产生特异性细胞毒性T细胞反应至关重要。

CD40 ligand is essential for generation of specific cytotoxic T cell responses in RNA-pulsed dendritic cell immunotherapy.

作者信息

Onaitis Mark W, Kalady Matthew F, Emani Sirisha, Abdel-Wahab Zeinab, Tyler Douglas S, Pruitt Scott K

机构信息

Department of Surgery, Duke University and Durham VA Medical Centers, Durham, NC 27710, USA.

出版信息

Surgery. 2003 Aug;134(2):300-5. doi: 10.1067/msy.2003.240.

DOI:10.1067/msy.2003.240
PMID:12947333
Abstract

BACKGROUND

Dendritic cell (DC)-based immunotherapy is a promising form of adjuvant therapy for high-risk tumors. DCs transfected with tumor-associated antigens are capable of stimulating antigen-specific T cells, but cytolytic responses have been disappointing. Activation of DC surface CD40 influences DC cytokine production, particularly that of interleukin (IL)-12, which favors a Th1 (cytotoxic) helper T cell response. This study evaluated the effects of exogenous soluble CD40 ligand (sCD40L) on RNA-transfected DC preparations and their subsequent ability to generate antimelanoma cytolytic T cells.

METHODS

Human monocyte-derived DCs were cultured and transfected with mRNA encoding full-length melanoma-associated antigen, Mart-1, and matured with and without sCD40L. DC IL-12 secretion and the ability to stimulate naïve T cells were assessed by enzyme-linked immunosorbent assay (ELISA), tetramer analysis, Elispot, and (51)Cr release assay.

RESULTS

Mature DCs stimulated with sCD40L secreted higher levels of IL-12 compared with immature DCs and DCs matured without sCD40L (P <.001). DCs treated with sCD40L generated a greater number of antigen-specific T cells (P <.05) by tetramer and Elispot analyses, and yielded specific T cells with significant cytotoxicity against HLA-matched melanoma cell lines.

CONCLUSIONS

CD40L augments DC IL-12 secretion and is essential to potentiate specific antimelanoma cytolytic responses stimulated by the Mart-1 antigen. sCD40L should be considered a crucial adjuvant in DC preparations for RNA-based DC vaccine therapies.

摘要

背景

基于树突状细胞(DC)的免疫疗法是一种有前景的高危肿瘤辅助治疗形式。用肿瘤相关抗原转染的DC能够刺激抗原特异性T细胞,但细胞溶解反应一直不尽人意。DC表面CD40的激活会影响DC细胞因子的产生,特别是白细胞介素(IL)-12的产生,这有利于Th1(细胞毒性)辅助性T细胞反应。本研究评估了外源性可溶性CD40配体(sCD40L)对RNA转染的DC制剂的影响及其随后产生抗黑色素瘤细胞溶解T细胞的能力。

方法

培养人单核细胞衍生的DC,用编码全长黑色素瘤相关抗原Mart-1的mRNA转染,并在有或没有sCD40L的情况下使其成熟。通过酶联免疫吸附测定(ELISA)、四聚体分析、酶联免疫斑点分析和(51)Cr释放测定评估DC的IL-12分泌以及刺激幼稚T细胞的能力。

结果

与未成熟DC和未用sCD40L成熟的DC相比,用sCD40L刺激的成熟DC分泌更高水平的IL-12(P<.001)。通过四聚体和酶联免疫斑点分析,用sCD40L处理的DC产生了更多的抗原特异性T细胞(P<.05),并产生了对HLA匹配的黑色素瘤细胞系具有显著细胞毒性的特异性T细胞。

结论

CD40L增强DC的IL-12分泌,并且对于增强由Mart-1抗原刺激的特异性抗黑色素瘤细胞溶解反应至关重要。在基于RNA的DC疫苗治疗的DC制剂中,sCD40L应被视为一种关键佐剂。

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