首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Dramatic increase in the numbers of functionally mature dendritic cells in Flt3 ligand-treated mice: multiple dendritic cell subpopulations identified
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Dramatic increase in the numbers of functionally mature dendritic cells in Flt3 ligand-treated mice: multiple dendritic cell subpopulations identified

机译:Flt3配体处理的小鼠中功能成熟的树突状细胞数量的急剧增加:确定了多个树突状细胞亚群

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摘要

Dendritic cells (DC) are the most efficient APC for T cells. The clinical use of DC as vectors for anti-tumor and infectious disease immunotherapy has been limited by their trace levels and accessibility in normal tissue and terminal state of differentiation. In the present study, daily injection of human Flt3 ligand (Flt3L) into mice results in a dramatic numerical increase in cells co-expressing the characteristic DC markers-class II MHC, CD11c, DEC205, and CD86. In contrast, in mice treated with either GM-CSF, GM-CSF plus IL-4, c-kit ligand (c-kitL), or G-CSF, class II+ CD11c+ cells were not significantly increased. Five distinct DC subpopulations were identified in the spleen of Flt3L-treated mice using CD8 alpha and CD11b expression. These cells exhibited veiled and dendritic processes and were as efficient as rare, mature DC isolated from the spleens of untreated mice at presenting allo-Ag or soluble Ag to T cells, or in priming an Ag-specific T cell response in vivo. Dramatic numerical increases in DC were detected in the bone marrow, gastro-intestinal lymphoid tissue (GALT), liver, lymph nodes, lung, peripheral blood, peritoneal cavity, spleen, and thymus. These results suggest that Flt3L could be used to expand the numbers of functionally mature DC in vivo for use in clinical immunotherapy.
机译:树突状细胞(DC)是T细胞最有效的APC。 DC作为抗肿瘤和传染病免疫治疗载体的临床应用受到其在正常组织中的痕量水平和可及性以及终末分化状态的限制。在本研究中,每天向小鼠注射人类Flt3配体(Flt3L)会导致细胞共表达特征性DC标记II类MHC,CD11c,DEC205和CD86的细胞数量急剧增加。相反,在用GM-CSF,GM-CSF加IL-4,c-kit配体(c-kitL)或G-CSF处理的小鼠中,II + CD11c +细胞没有明显增加。使用CD8α和CD11b表达,在Flt3L处理的小鼠的脾脏中鉴定出五个不同的DC亚群。这些细胞表现出遮盖的和树突状的过程,并且与从未处理的小鼠脾脏中分离出的稀有成熟DC一样有效,可以将异源Ag或可溶性Ag呈现给T细胞,或在体内引发Ag特异性T细胞反应。在骨髓,胃肠道淋巴样组织(GALT),肝,淋巴结,肺,外周血,腹膜腔,脾脏和胸腺中检测到DC的数字显着增加。这些结果表明,Flt3L可用于扩大体内功能成熟的DC的数量,以用于临床免疫治疗。

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