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表达粒细胞巨噬细胞集落刺激因子的质粒疫苗会吸引包括未成熟树突状细胞在内的浸润细胞进入注射的肌肉。

Plasmid vaccine expressing granulocyte-macrophage colony-stimulating factor attracts infiltrates including immature dendritic cells into injected muscles.

作者信息

Haddad D, Ramprakash J, Sedegah M, Charoenvit Y, Baumgartner R, Kumar S, Hoffman S L, Weiss W R

机构信息

Malaria Program, Naval Medical Research Center, Silver Spring, MD 20910, USA.

出版信息

J Immunol. 2000 Oct 1;165(7):3772-81. doi: 10.4049/jimmunol.165.7.3772.

DOI:10.4049/jimmunol.165.7.3772
PMID:11034382
Abstract

Plasmid-encoded GM-CSF (pGM-CSF) is an adjuvant for genetic vaccines; however, little is known about how pGM-CSF enhances immunogenicity. We now report that pGM-CSF injected into mouse muscle leads to a local infiltration of potential APCs. Infiltrates reached maximal size on days 3 to 5 after injection and appeared in several large discrete clusters within the muscle. Immunohistological studies in muscle sections from mice injected with pGM-CSF showed staining of cells with the macrophage markers CD11b, Mac-3, IA(d)/E(d) and to the granulocyte marker GR-1 from day 1 through day 14. Cells staining with the dendritic cell marker CD11c were detected only on days 3 to 5. Muscles injected with control plasmids did not stain for CD11c but did stain for CD11b, Mac-3, IA(d)/E(d), and GR-1. No staining was observed with the APC activation markers, B7.1 or CD40, or with markers for T or B cells. These findings are consistent with the infiltrating cells in the pGM-CSF-injected muscles being a mixture of neutrophils, macrophages, and immature dendritic cells and suggest that the i.m. APCs may be enhancing immune responses to coinjected plasmid Ags. This hypothesis is supported by data showing that 1) separation of injections with pGM-CSF and Ag-expressing plasmid into different sites did not enhance immune responses and 2) immune enhancement was associated with the presence of CD11c+ cells in the infiltrates. Thus, pGM-CSF enhancement may depend on APC recruitment to the i.m. site of injection.

摘要

质粒编码的粒细胞-巨噬细胞集落刺激因子(pGM-CSF)是基因疫苗的一种佐剂;然而,关于pGM-CSF如何增强免疫原性却知之甚少。我们现在报告,注入小鼠肌肉的pGM-CSF会导致潜在抗原呈递细胞(APC)的局部浸润。注射后第3至5天,浸润细胞达到最大规模,并在肌肉内呈现为几个大的离散簇。对注射pGM-CSF的小鼠肌肉切片进行的免疫组织学研究显示,从第1天到第14天,细胞被巨噬细胞标志物CD11b、Mac-3、IA(d)/E(d)以及粒细胞标志物GR-1染色。仅在第3至5天检测到被树突状细胞标志物CD11c染色的细胞。注射对照质粒的肌肉未被CD11c染色,但被CD11b、Mac-3、IA(d)/E(d)和GR-1染色。未观察到APC激活标志物B7.1或CD40以及T或B细胞标志物的染色。这些发现与注射pGM-CSF的肌肉中的浸润细胞是中性粒细胞、巨噬细胞和未成熟树突状细胞的混合物一致,并表明肌肉内的APC可能增强对共注射质粒抗原的免疫反应。这一假设得到以下数据的支持:1)将pGM-CSF注射与表达抗原的质粒注射分隔到不同部位并不能增强免疫反应;2)免疫增强与浸润物中CD11c+细胞的存在相关。因此,pGM-CSF的增强作用可能取决于APC募集到肌肉注射部位。

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