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Hepatitis B core protein as a therapeutic target

机译:乙型肝炎核心蛋白作为治疗靶标

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Introduction: Chronic hepatitis B virus (HBV) infection is difficult to cure, due to the presence of covalently-closed-circular DNA and virus-mediated blunting of host immune response. Existing therapies with nucleos(t)ide analogue or pegylated-interferon are not sufficient to achieve a high rate of HBV surface antigen seroclearance, a more desirable treatment outcome. Novel therapeutic agents targeting alternative viral replication steps are being developed. In this review, we will discuss the hepatitis B core antigen (HBcAg) as a therapeutic target.Areas covered: The basic structure and fundamental functions of HBcAg including nucleocapsid assembly, pre-genomic RNA encapsidation, reverse transcription, virion formation, cccDNA amplification, immune response regulation, and HBx protein interaction will be reviewed. Most of these are identified as therapeutic targets and tested in in vitro and in vivo studies, although clinical trials are scanty. Among the different components, the core protein allosteric modulators (CpAM) have been most widely investigated and appear promising in clinical trials.Expert opinion: The multiple and essential functions of HBcAg for HBV life cycle are important and attractive targets for HBV therapeutic interventions. Controlled trials involving CpAM are awaited. Apart from CpAM, drugs directed against different functions of HBcAg may be further explored to maximize the chance of cure.
机译:介绍:由于存在共价闭合的圆形DNA和病毒介导的宿主免疫应答的病毒介导的核心,慢性乙型肝炎病毒(HBV)感染难以治愈。与核型(T)IDE类似物或聚乙二醇化干扰素的现有疗法不足以实现高速率的HBV表面抗原血清性,更期望的治疗结果。正在开发出靶向替代病毒复制步骤的新型治疗剂。在本综述中,我们将讨论乙型肝炎核心抗原(HBCAG)作为治疗目标。覆盖:HBCAG的基本结构和基本功能,包括核衣壳组装,预转录前的RNA封装,逆转录,病毒肾形成,CCCDNA扩增,将审查免疫响应调控和HBX蛋白质互动。其中大多数这些被鉴定为治疗靶标并在体外测试和体内研究,尽管临床试验很少。在不同的组分中,核心蛋白血糖蛋白调节剂(CPAM)最被广泛研究,并且在临床试验中似乎很有前景。普及意见:HBV终生命周期的HBCAG的多项和基本功能是HBV治疗干预的重要性和有吸引力的目标。等待了涉及CPAM的受控试验。除CPAM外,还可以进一步探索针对HBCAG的不同功能的药物,以最大限度地提高固化的机会。

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