感染猫免疫缺陷病毒的猫中T细胞启动和增殖受损。
Impaired T-cell priming and proliferation in cats infected with feline immunodeficiency virus.
作者信息
Bishop S A, Williams N A, Gruffydd-Jones T J, Harbour D A, Stokes C R
机构信息
Department of Veterinary Medicine, University of Bristol, UK.
出版信息
AIDS. 1992 Mar;6(3):287-93. doi: 10.1097/00002030-199203000-00005.
OBJECTIVE
Cats naturally infected with feline immunodeficiency virus (FIV) are particularly susceptible to infection with opportunistic pathogens, suggesting that these animals are unable to develop an effective immune response against the pathogen. Previous studies have used CD4+:CD8+ lymphocyte ratios and mitogen blastogenesis to identify immunological abnormalities in FIV-infected cats. However, these studies provide limited information for understanding the nature of the cellular dysfunction in FIV-infected cats, particularly defects in antigen-specific immune responses.
DESIGN
To investigate whether cats infected with FIV are less able to mount an immune response to previously unencountered antigens, we compared the development of antigen-specific cellular immunity at the stage of T-cell priming in uninfected and FIV-infected cats.
INTERVENTIONS
The general immune status of cats was assessed by peripheral blood CD4+:CD8+ lymphocyte ratios (flow cytometry), and by lymphocyte blastogenesis response to T- and B-cell mitogens. In addition, we describe the development of an autologous culture system to measure specific priming of naive feline T-cells to soluble antigen in vitro. This assay was used to compare T-cell priming in uninfected cats and cats which had been infected with FIV for 6-27 months.
RESULTS
As in HIV infection, CD4+:CD8+ lymphocyte ratios in FIV-infected cats were found to be inverted, due to a reduction in the percentage of CD4+ cells. In addition, lymphocyte blastogenesis to both T- and B-cell mitogens was significantly impaired in FIV-infected cats. Priming to keyhole limpet haemocyanin (KLH) elicited a late proliferative response resulting from the expansion of CD4+ (T-helper cells). T-cell growth factor secretion correlated with cell proliferation. Restimulation of cells with fresh antigen-presenting cells and antigen showed that antigen-specific T-cell priming had occurred in the initial culture. When primary proliferation responses in FIV-infected cats were examined, it was observed that naive CD4+ T-cells from FIV-infected cats were significantly impaired (P less than 0.001) in their ability to be primed to KLH when compared with uninfected controls.
CONCLUSIONS
Impaired priming of naive CD4+ T-helper cells to antigen in FIV-infected cats may explain the increased susceptibility of these animals to infection by opportunistic pathogens. The poor ability of human patients with AIDS to develop humoral immunity following vaccination may also be caused by such a defect in T-cell priming.
目的
自然感染猫免疫缺陷病毒(FIV)的猫对机会性病原体感染特别易感,这表明这些动物无法对病原体产生有效的免疫反应。以往的研究利用CD4⁺:CD8⁺淋巴细胞比率和丝裂原刺激的细胞增殖来确定FIV感染猫的免疫异常。然而,这些研究对于理解FIV感染猫细胞功能障碍的本质,尤其是抗原特异性免疫反应缺陷,提供的信息有限。
设计
为了研究感染FIV的猫对先前未接触过的抗原产生免疫反应的能力是否降低,我们比较了未感染和FIV感染猫在T细胞致敏阶段抗原特异性细胞免疫的发展情况。
干预措施
通过外周血CD4⁺:CD8⁺淋巴细胞比率(流式细胞术)以及淋巴细胞对T细胞和B细胞丝裂原的增殖反应来评估猫的一般免疫状态。此外,我们描述了一种自体培养系统的建立,用于在体外测量幼稚猫T细胞对可溶性抗原的特异性致敏。该试验用于比较未感染猫和感染FIV 6 - 27个月的猫的T细胞致敏情况。
结果
与HIV感染一样,发现FIV感染猫的CD4⁺:CD8⁺淋巴细胞比率倒置,原因是CD4⁺细胞百分比降低。此外,FIV感染猫对T细胞和B细胞丝裂原的淋巴细胞增殖反应均显著受损。对钥孔戚血蓝蛋白(KLH)的致敏引发了由CD4⁺(辅助性T细胞)扩增导致的晚期增殖反应。T细胞生长因子分泌与细胞增殖相关。用新鲜抗原呈递细胞和抗原对细胞进行再刺激表明,在初始培养中已发生抗原特异性T细胞致敏。当检查FIV感染猫的初次增殖反应时,发现与未感染对照相比,FIV感染猫的幼稚CD4⁺T细胞对KLH的致敏能力显著受损(P<0.001)。
结论
FIV感染猫中幼稚CD4⁺辅助性T细胞对抗原的致敏受损可能解释了这些动物对机会性病原体感染易感性增加的原因。艾滋病患者接种疫苗后体液免疫能力差也可能是由T细胞致敏缺陷所致。
Zotero 插件