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用树突状细胞进行丙型肝炎病毒感染的预防性和治疗性疫苗接种。

Prophylactic and therapeutic vaccination with dendritic cells against hepatitis C virus infection.

作者信息

Encke J, Findeklee J, Geib J, Pfaff E, Stremmel W

机构信息

Department of Internal Medicine IV, University of Heidelberg, Germany.

出版信息

Clin Exp Immunol. 2005 Nov;142(2):362-9. doi: 10.1111/j.1365-2249.2005.02919.x.

Abstract

Antigen uptake and presentation capacities enable DC to prime and activate T cells. Recently, several studies demonstrated a diminished DC function in hepatitis C virus (HCV) infected patients showing impaired abilities to stimulate allogenic T cells and to produce IFN-gamma in HCV infected patients. Moreover, DC of patients who have resolved HCV infection behave like DC from healthy donors responding to maturation stimuli, decrease antigen uptake, up-regulate expression of appropriate surface marker, and are potent stimulators of allogenic T cells. A number of studies have demonstrated in tumour models and models of infectious diseases strong induction of immune responses after DC vaccination. Because DC are essential for T-cell activation and since viral clearance in HCV infected patients is associated with a vigorous T-cell response, we propose a new type of HCV vaccine based on ex vivo stimulated and matured DC loaded with HCV specific antigens. This vaccine circumvents the impaired DC maturation and the down regulated DC function of HCV infected patients in vivo by giving the necessary maturation stimuli and the HCV antigens in a different setting and location ex vivo. Strong humoral and cellular immune responses were detected after HCV core DC vaccination. Furthermore, DC vaccination shows partial protection in a therapeutic and prophylactic model of HCV infection. In conclusion, mice immunized with HCV core pulsed DC generated a specific antiviral response in a mouse HCV challenge model. Our results indicate that HCV core pulsed DC may serve as a new modality for immunotherapy of HCV especially in chronically infected patients.

摘要

抗原摄取和呈递能力使树突状细胞(DC)能够启动和激活T细胞。最近,多项研究表明,丙型肝炎病毒(HCV)感染患者的DC功能减弱,表现为刺激同种异体T细胞以及在HCV感染患者中产生γ干扰素的能力受损。此外,已清除HCV感染的患者的DC表现得如同来自健康供体的DC,对成熟刺激有反应,减少抗原摄取,上调适当表面标志物的表达,并且是同种异体T细胞的有效刺激剂。许多研究已在肿瘤模型和传染病模型中证明,DC疫苗接种后可强烈诱导免疫反应。由于DC对T细胞激活至关重要,且HCV感染患者中的病毒清除与强烈的T细胞反应相关,我们提出一种新型的HCV疫苗,该疫苗基于负载有HCV特异性抗原的体外刺激和成熟的DC。这种疫苗通过在体外不同环境和位置给予必要的成熟刺激和HCV抗原,规避了HCV感染患者体内DC成熟受损和DC功能下调的问题。HCV核心DC疫苗接种后检测到强烈的体液和细胞免疫反应。此外,DC疫苗接种在HCV感染的治疗和预防模型中显示出部分保护作用。总之,用HCV核心脉冲DC免疫的小鼠在小鼠HCV攻击模型中产生了特异性抗病毒反应。我们的结果表明,HCV核心脉冲DC可能成为HCV免疫治疗的一种新方式,尤其是对于慢性感染患者。

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