Löhr H F, Pingel S, Böcher W O, Bernhard H, Herzog-Hauff S, Rose-John S, Galle P R
Department of Internal Medicine, Johannes-Gutenberg-University Mainz, Mainz, Germany.
Clin Exp Immunol. 2002 Oct;130(1):107-14. doi: 10.1046/j.1365-2249.2002.01943.x.
Insufficient stimulatory capacities of autologous dendritic cells (DC) may contribute in part to impaired T cell stimulation and therefore viral persistence in patients with chronic hepatitis B virus (HBV) infection. In order to characterize the antigen presenting functions of DC from chronic HBV carriers and controls antigen specific T cell responses were analysed. CD34+ peripheral blood progenitor cells were differentiated to immature DC in the presence of GM-CSF, IL-6/IL-6R fusion protein and stem cell factor. Proliferative CD4+ T cell responses and specific cytokine release were analysed in co-cultures of DC pulsed with HBV surface and core antigens or tetanus toxoid and autologous CD4+ T cells. Cultured under identical conditions DC from chronic HBV carriers, individuals with acute resolved hepatitis B and healthy controls expressed similar phenotypical markers but chronic HBV carriers showed less frequent and weaker HBV antigen specific proliferative T helper cell responses and secreted less interferon-gamma while responses to the tetanus toxoid control antigen was not affected. Preincubation with recombinant IL-12 enhanced the HBV specific immune reactivities in chronic HBV patients and controls. In conclusion, the weak antiviral immune responses observed in chronic hepatitis B may result in part from insufficient T cell stimulating capacities of DC. Immunostimulation by IL-12 restored the HBV antigen specific T cell responses and could have some therapeutical benefit to overcome viral persistence.
自体树突状细胞(DC)刺激能力不足可能部分导致慢性乙型肝炎病毒(HBV)感染患者的T细胞刺激受损,进而导致病毒持续存在。为了表征慢性HBV携带者和对照的DC的抗原呈递功能,分析了抗原特异性T细胞反应。在GM-CSF、IL-6/IL-6R融合蛋白和干细胞因子存在的情况下,将CD34+外周血祖细胞分化为未成熟DC。在用HBV表面和核心抗原或破伤风类毒素脉冲处理的DC与自体CD4+T细胞的共培养物中,分析增殖性CD4+T细胞反应和特异性细胞因子释放。在相同条件下培养的慢性HBV携带者、急性乙型肝炎康复个体和健康对照的DC表达相似的表型标志物,但慢性HBV携带者的HBV抗原特异性增殖性T辅助细胞反应频率较低且较弱,分泌的干扰素-γ较少,而对破伤风类毒素对照抗原的反应不受影响。用重组IL-12预孵育可增强慢性HBV患者和对照中的HBV特异性免疫反应性。总之,慢性乙型肝炎中观察到的弱抗病毒免疫反应可能部分源于DC的T细胞刺激能力不足。IL-12免疫刺激恢复了HBV抗原特异性T细胞反应,可能对克服病毒持续存在具有一定的治疗益处。