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Characterization of Lymphocyte Response in the Female Genital Tract during Ascending Chlamydial Genital Infection in the Guinea Pig Model

机译:豚鼠模型中衣原体生殖道感染上升过程中女性生殖道淋巴细胞反应的表征

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摘要

It is well known that pathology caused by chlamydial infection is associated closely with the host response to the organism and that both innate and adaptive host responses contribute to tissue damage. While it is likely that the organism itself initiates the acute inflammatory response by eliciting cytokine and chemokine production from the host cell, the adaptive response is the result of activation of the cell-mediated immune response. While there are several studies describing the nature of the pathologic response in primate, guinea pig, and murine models, there is less information on the kinetics of the CD4 and CD8 response following primary and challenge infections. In this study, we have quantified by flow cytometry the mononuclear cell response to genital infection with the agent of guinea pig inclusion conjunctivitis in the cervix, endometrium, and oviducts at various times following a primary intravaginal infection and after a challenge infection. Tissues from individual animals were assessed for cells expressing CD4, CD8, or Mac-1 and for B cells. Peak responses of each subset occurred 10 to 14 days after a primary infection. The number of Mac-1-expressing cells in each tissue site was found to be dependent on the size of the inoculating dose of chlamydiae. The responses of each cell type were generally stronger in the cervix than in the upper genital tract. In contrast to the murine model but consistent with the primate models, there were equal numbers of CD4 and CD8 cells present in the infiltrates. Twenty-one days after challenge infection, which was performed 50 days after the primary infection, there was a significant increase in the number of CD4, CD8, and B cells in the oviduct compared to the number of these cells at the same time after a primary infection, providing clear cellular evidence for a cell-mediated immune pathologic response.
机译:众所周知,衣原体感染引起的病理与宿主对生物体的反应密切相关,先天性和适应性宿主反应均导致组织损伤。虽然有机体本身可能通过引起宿主细胞引起细胞因子和趋化因子的产生而引发急性炎症反应,但适应性反应是细胞介导的免疫反应激活的结果。尽管有几项研究描述了灵长类,豚鼠和鼠模型中病理反应的性质,但有关原发性感染和攻击性感染后CD4和CD8响应动力学的信息较少。在这项研究中,我们已通过流式细胞术量化了在初次阴道内感染和攻击性感染后不同时间,豚鼠包涵体结膜炎对子宫颈,子宫内膜和输卵管中生殖器感染的单核细胞反应。评价来自个体动物的组织的表达CD4,CD8或Mac-1的细胞和B细胞。初次感染后10到14天,每个子集的反应高峰。发现每个组织部位中表达Mac-1的细胞数量取决于衣原体接种剂量的大小。每种细胞类型的反应通常在子宫颈中比在上生殖道中更强。与鼠模型相反但与灵长类动物模型一致,浸润液中存在相等数量的CD4和CD8细胞。在初次感染后的第50天进行攻击感染后的21天,输卵管中CD4,CD8和B细胞的数量比一次感染后同时出现的数量显着增加。原发性感染,为细胞介导的免疫病理反应提供了清晰的细胞证据。

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