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沙门氏菌能有效地进入培养的CD11c+树突状细胞并在其中存活,从而启动细胞因子表达。

Salmonella efficiently enter and survive within cultured CD11c+ dendritic cells initiating cytokine expression.

作者信息

Marriott I, Hammond T G, Thomas E K, Bost K L

机构信息

Department of Biology, University of North Carolina at Charlotte, 28223, USA.

出版信息

Eur J Immunol. 1999 Apr;29(4):1107-15. doi: 10.1002/(SICI)1521-4141(199904)29:04<1107::AID-IMMU1107>3.0.CO;2-0.

Abstract

While Salmonella infects macrophages, this cell population may not be the only one important for disseminating intracellular bacteria from mucosal sites. Dendritic cells (DC) are present in the Peyer's patches and are mobilized following stimulation. Such characteristics would seem to be ideal for the dissemination of an intracellular, mucosal pathogen. However, it has been difficult to obtain sufficient numbers of DC to assess their ability to harbor Salmonella or to monitor DC in vivo. In the present study, this problem has been addressed by expanding DC in vivo using flt3 ligand, followed by the purification of CD11c+ cells using antibody-coated magnetic beads or by fluorescence-activated cell sorting. Salmonella dublin were found to be efficiently internalized, and to survive and replicate within purified CD11c+ DC, and also in CD11c+, CD8alpha+ or CD11c+, CD11b+ DC subpopulations. The ability of Salmonella to enter DC is of similar magnitude to that reported for macrophages, suggesting that this cell population could be an important host cell for dissemination of this pathogen from mucosal sites. Furthermore, infected DC responded to Salmonella by secretion of IL-1, IL-6 and IL-12. As such, these cells may be important sources of these cytokines during the host response against Salmonella infection.

摘要

虽然沙门氏菌会感染巨噬细胞,但这群细胞可能并非唯一对从黏膜部位播散细胞内细菌至关重要的细胞。树突状细胞(DC)存在于派尔集合淋巴结中,并在受到刺激后被动员起来。这些特性似乎对于细胞内黏膜病原体的播散而言是理想的。然而,一直以来很难获得足够数量的DC来评估它们容纳沙门氏菌的能力或在体内监测DC。在本研究中,通过使用Flt3配体在体内扩增DC,随后使用抗体包被的磁珠或荧光激活细胞分选法纯化CD11c⁺细胞,解决了这个问题。发现都柏林沙门氏菌能被有效地内化,并在纯化的CD11c⁺DC内以及CD11c⁺、CD8α⁺或CD11c⁺、CD11b⁺DC亚群内存活和复制。沙门氏菌进入DC的能力与报道的巨噬细胞的能力相似,这表明这群细胞可能是该病原体从黏膜部位播散的重要宿主细胞。此外,受感染的DC通过分泌IL-1、IL-6和IL-12对沙门氏菌作出反应。因此,在宿主针对沙门氏菌感染的反应过程中,这些细胞可能是这些细胞因子的重要来源。

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