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Antigen Presentation Capacity and Cytokine Production by Murine Splenic Dendritic Cell Subsets upon Salmonella Encounter

机译:沙门氏菌遭遇鼠脾树突状细胞亚群的抗原提呈能力和细胞因子的生产。

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Salmonella typhimurium is an intracellular bacterium that replicates in the spleen and mesenteric lymph nodes (MLN) of orally infected mice. However, little is known about the Ag presentation and cytokine production capacity of dendritic cells (DC), particularly CD8α+, CD8α?CD4?, and CD8α?CD4+ DC, from these organs in response to Salmonella . Infection of purified splenic DC with S. typhimiurium expressing green fluorescent protein (GFP) and OVA revealed that all three splenic DC subsets internalize bacteria, and splenic as well as MLN DC process Salmonella for peptide presentation. Furthermore, presentation of Salmonella Ags on MHC-I and MHC-II was evident in both CD8α+ and CD8α? splenic DC subsets. Direct ex vivo analysis of splenic DC from mice infected with GFP-expressing Salmonella showed that all three subsets harbored bacteria, and splenic DC purified from mice given Salmonella -expressing OVA presented OVA-derived peptides on MHC-I and MHC-II. Cytokine production analyzed by intracellular staining of splenic DC infected with GFP-expressing Salmonella revealed that TNF-α was produced by a large percentage of CD8α? DC, while only a minor proportion of CD8α+ DC produced this cytokine following bacterial exposure. In contrast, the greatest number of IL-12p40-producing DC were among CD8α+ DC. Experiments inhibiting bacterial uptake by cytochalasin D as well as use of a Transwell system revealed that bacterial contact, but not internalization, was required for cytokine production. Thus, DC in sites of Salmonella replication and T cell activation, spleen and MLN, respond to bacterial encounter by Ag presentation and produce cytokines in a subset-specific fashion.
机译:鼠伤寒沙门氏菌是一种细胞内细菌,可在口腔感染小鼠的脾脏和肠系膜淋巴结(MLN)中复制。但是,关于这些植物响应沙门氏菌的抗原呈递和树突状细胞(DC),特别是CD8α+,CD8ααCD4α和CD8αβCD4+ DC的细胞因子生产能力知之甚少。纯化的脾脏DC用表达绿色荧光蛋白(GFP)的鼠伤寒沙门氏菌和OVA感染后发现,这三个脾脏DC子集都将细菌内在化,脾脏以及MLN DC处理沙门氏菌以呈递肽。此外,在CD8α+和CD8αβ中,沙门氏菌Ags在MHC-I和MHC-II上的表达是明显的。脾脏DC子集。从表达GFP的沙门氏菌感染的小鼠的脾脏DC的直接离体分析表明,所有三个亚群都携带细菌,并且从给予表达沙门氏菌的OVA的小鼠纯化的脾脏DC在MHC-1和MHC-II上呈现OVA衍生的肽。通过用表达GFP的沙门氏菌感染的脾脏DC进行细胞内染色分析的细胞因子产生表明,TNF-α是由大部分CD8αβ产生的。 DC,而细菌接触后只有一小部分CD8α+ DC产生这种细胞因子。相反,在CD8α+ DC中,产生IL-12p40的DC最多。抑制细胞松弛素D吸收细菌的实验以及Transwell系统的使用表明,细胞因子的产生需要细菌的接触而不是内在化。因此,沙门氏菌复制和T细胞活化,脾脏和MLN部位的DC通过Ag呈递对细菌的接触作出反应,并以亚群特异性方式产生细胞因子。

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