MHC I类提出T细胞表位作为抗HBV慢性感染治疗性疫苗的潜在抗原

Hepatitis research and treatment Pub Date : 2014-01-01 Epub Date: 2014-05-26 DOI:10.1155/2014/860562
Joseph D Comber, Aykan Karabudak, Vivekananda Shetty, James S Testa, Xiaofang Huang, Ramila Philip
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引用次数: 21

摘要

全世界约有3.7亿人慢性感染乙型肝炎病毒(HBV)。尽管预防性HBV疫苗取得了成功,但没有治疗性疫苗或其他免疫治疗方式可用于治疗慢性感染者。HBV的清除依赖于强劲、持续的CD8(+) T活性;然而,试验过的数量有限的治疗性疫苗并没有引起这种反应。这些疫苗大多依赖于肽预测算法来识别MHC-I表位或表征急性感染期间的T细胞反应。在这里,我们采用免疫蛋白质组学方法来表征慢性HBV感染细胞的MHC-I限制性表位,因此更有可能代表慢性感染期间CD8(+) T细胞的真正靶标。在这项研究中,我们鉴定了八个新的MHC-I限制性表位,这些表位来源于广泛的HBV蛋白,能够激活CD8(+) T细胞。此外,8个表位中的5个能够结合HLA-A2和A24等位基因并激活HBV特异性T细胞反应。这些表位也有潜力作为表征慢性HBV感染中T细胞免疫的新工具,并可能作为抗HBV感染治疗性疫苗的候选抗原。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

MHC Class I Presented T Cell Epitopes as Potential Antigens for Therapeutic Vaccine against HBV Chronic Infection.

MHC Class I Presented T Cell Epitopes as Potential Antigens for Therapeutic Vaccine against HBV Chronic Infection.

MHC Class I Presented T Cell Epitopes as Potential Antigens for Therapeutic Vaccine against HBV Chronic Infection.

MHC Class I Presented T Cell Epitopes as Potential Antigens for Therapeutic Vaccine against HBV Chronic Infection.

Approximately 370 million people worldwide are chronically infected with hepatitis B virus (HBV). Despite the success of the prophylactic HBV vaccine, no therapeutic vaccine or other immunotherapy modality is available for treatment of chronically infected individuals. Clearance of HBV depends on robust, sustained CD8(+) T activity; however, the limited numbers of therapeutic vaccines tested have not induced such a response. Most of these vaccines have relied on peptide prediction algorithms to identify MHC-I epitopes or characterization of T cell responses during acute infection. Here, we took an immunoproteomic approach to characterize MHC-I restricted epitopes from cells chronically infected with HBV and therefore more likely to represent the true targets of CD8(+) T cells during chronic infection. In this study, we identified eight novel MHC-I restricted epitopes derived from a broad range of HBV proteins that were capable of activating CD8(+) T cells. Furthermore, five of the eight epitopes were able to bind HLA-A2 and A24 alleles and activated HBV specific T cell responses. These epitopes also have potential as new tools to characterize T cell immunity in chronic HBV infection and may serve as candidate antigens for a therapeutic vaccine against HBV infection.

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