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药物滥用、人类免疫缺陷病毒1型与肝炎

Substance abuse, HIV-1 and hepatitis.

作者信息

Parikh Nirzari, Nonnemacher Michael R, Pirrone Vanessa, Block Timothy, Mehta Anand, Wigdahl Brian

机构信息

Department of Microbiology and Immunology, Drexel University College of Medicine, Philadelphia, PA 19102, USA.

出版信息

Curr HIV Res. 2012 Oct;10(7):557-71. doi: 10.2174/157016212803306023.

Abstract

During the course of human immunodeficiency virus type 1 (HIV-1) disease, the virus has been shown to effectively escape the immune response with the subsequent establishment of latent viral reservoirs in specific cell populations within the peripheral blood (PB) and associated lymphoid tissues, bone marrow (BM), brain, and potentially other end organs. HIV-1, along with hepatitis B and C viruses (HBV and HCV), are known to share similar routes of transmission, including intravenous drug use, blood transfusions, sexual intercourse, and perinatal exposure. Substance abuse, including the use of opioids and cocaine, is a significant risk factor for exposure to HIV-1 and the development of acquired immune deficiency syndrome, as well as HBV and HCV exposure, infection, and disease. Thus, coinfection with HIV-1 and HBV or HCV is common and may be impacted by chronic substance abuse during the course of disease. HIV- 1 impacts the natural course of HBV and HCV infection by accelerating the progression of HBV/HCV-associated liver disease toward end-stage cirrhosis and quantitative depletion of the CD4+ T-cell compartment. HBV or HCV coinfection with HIV-1 is also associated with increased mortality when compared to either infection alone. This review focuses on the impact of substance abuse and coinfection with HBV and HCV in the PB, BM, and brain on the HIV-1 pathogenic process as it relates to viral pathogenesis, disease progression, and the associated immune response during the course of this complex interplay. The impact of HIV-1 and substance abuse on hepatitis virus-induced disease is also a focal point.

摘要

在1型人类免疫缺陷病毒(HIV-1)疾病进程中,已证实该病毒能有效逃避免疫反应,随后在外周血(PB)及相关淋巴组织、骨髓(BM)、脑以及可能的其他终末器官中的特定细胞群体中建立潜伏病毒库。已知HIV-1与乙型和丙型肝炎病毒(HBV和HCV)具有相似的传播途径,包括静脉吸毒、输血、性交和围产期暴露。药物滥用,包括使用阿片类药物和可卡因,是感染HIV-1以及发展为获得性免疫缺陷综合征的重要危险因素,也是接触HBV和HCV、感染及发病的重要危险因素。因此,HIV-1与HBV或HCV合并感染很常见,且在疾病过程中可能受到慢性药物滥用的影响。HIV-1通过加速HBV/HCV相关肝病向终末期肝硬化的进展以及CD4+T细胞区室的数量减少,影响HBV和HCV感染的自然病程。与单独感染相比,HBV或HCV与HIV-1合并感染还与死亡率增加相关。本综述重点关注PB、BM和脑中药物滥用以及HBV和HCV合并感染对HIV-1致病过程的影响,这涉及到这种复杂相互作用过程中的病毒发病机制、疾病进展及相关免疫反应。HIV-1和药物滥用对肝炎病毒所致疾病的影响也是一个重点。

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