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增强恒河猴树突状细胞的体外刺激以激活SIV特异性T细胞反应。

Enhanced in vitro stimulation of rhesus macaque dendritic cells for activation of SIV-specific T cell responses.

作者信息

Mehlhop Erin, Villamide Loreley A, Frank Ines, Gettie Agegnehu, Santisteban Christine, Messmer Davorka, Ignatius Ralf, Lifson Jeffrey D, Pope Melissa

机构信息

Laboratory of Cellular Physiology and Immunology, The Rockefeller University, 1230 York Avenue, New York, NY 10021, USA.

出版信息

J Immunol Methods. 2002 Feb 1;260(1-2):219-34. doi: 10.1016/s0022-1759(01)00544-0.

Abstract

The macaque-simian immunodeficiency virus (SIV) system is one of the best animal models available to study the role of dendritic cells (DCs) in transmission and pathogenesis of HIV, as well as to test DC-based vaccine and therapeutic strategies. To better define and optimize this system, the responsiveness of macaque monocyte-derived DCs to a variety of maturation stimuli was examined. Characteristic immunophenotypic and functional DC maturation induced by standard monocyte conditioned medium (MCM) was compared to the activation induced by a panel of stimuli including soluble CD40L, LPS, Poly I:C, PGE(2)/TNFalpha, and a cocktail mixture of PGE(2)/TNFalpha/IL-1beta/IL-6. Immunophenotypic analysis confirmed that all stimuli induced stable up-regulation of CD25, CD40, CD80, CD83, CD86, HLA-DR, DC-LAMP (CD208), and DEC-205 (CD205). In general, macaque DCs exhibited weaker responses to LPS and Poly I:C than human DCs, and soluble CD40L stimulation induced variable expression of CD25. Interestingly, while the endocytic capacity of CD40L-matured cells was down-modulated comparably to DCs matured with MCM or the cocktail, the T cell stimulatory activity was not enhanced to the same extent. The particularly reproducible and potent T cell stimulatory capacity of cocktail-treated DCs correlated with a more homogenous mature DC phenotype, consistently high levels of IL-12 production, and better viability upon reculture compared to DCs activated by other stimuli. Furthermore, cocktail-matured DCs efficiently captured and presented inactivated SIV to SIV-primed T cells in vitro. Thus, the cocktail represents a particularly potent and useful stimulus for the generation of efficacious immunostimulatory macaque DCs.

摘要

猕猴 - 猴免疫缺陷病毒(SIV)系统是研究树突状细胞(DCs)在HIV传播和发病机制中的作用以及测试基于DC的疫苗和治疗策略的最佳动物模型之一。为了更好地定义和优化该系统,研究了猕猴单核细胞衍生的DCs对多种成熟刺激的反应性。将标准单核细胞条件培养基(MCM)诱导的特征性免疫表型和功能性DC成熟与包括可溶性CD40L、LPS、Poly I:C、PGE(2)/TNFα以及PGE(2)/TNFα/IL-1β/IL-6混合鸡尾酒在内的一组刺激诱导的激活进行了比较。免疫表型分析证实,所有刺激均诱导CD25、CD40、CD80、CD83、CD86、HLA-DR、DC-LAMP(CD208)和DEC-205(CD205)的稳定上调。一般来说,猕猴DCs对LPS和Poly I:C的反应比人类DCs弱,可溶性CD40L刺激诱导CD25的表达可变。有趣的是,虽然CD40L成熟细胞的内吞能力与用MCM或混合鸡尾酒成熟的DCs相比下调程度相当,但T细胞刺激活性并未增强到相同程度。与其他刺激激活的DCs相比,混合鸡尾酒处理的DCs特别可重复且强大的T细胞刺激能力与更均匀的成熟DC表型、持续高水平的IL-12产生以及再培养时更好的活力相关。此外,混合鸡尾酒成熟的DCs在体外有效地捕获并将灭活的SIV呈递给经SIV致敏的T细胞。因此,混合鸡尾酒是产生有效的免疫刺激猕猴DCs的特别有效和有用的刺激物。

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