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Epidemiology, pathogenesis and management of hepatitis D: update and challenges ahead.

机译:丁型肝炎的流行病学,发病机制和管理:最新动态和面临的挑战。

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Hepatitis D is caused by infection with the hepatitis D virus (HDV) and is considered to be the most severe form of viral hepatitis in humans. Hepatitis D occurs only in individuals positive for the HBV surface antigen (HBsAg) as HDV is a defective RNA viroid that requires HBsAg for transmission. At least eight different HDV genotypes have been described and each has a characteristic geographic distribution and a distinct clinical course. HDV and HBV coinfection can be associated with complex and dynamic viral dominance patterns. Chronic HDV infection leads to more severe liver disease than HBV monoinfection and is associated with accelerated fibrosis progression, earlier hepatic decompensation and an increased risk for the development of hepatocellular carcinoma. So far, only IFN-alpha treatment has proven antiviral activity against HDV in humans and has been linked to improved long-term outcomes. Studies conducted in the past 2 years on the use of PEG-IFN-alpha show that a sustained virologic response to therapy, measured in terms of undetectable serum HDV RNA levels, can be achieved in about one quarter of patients with hepatitis D. Novel alternative treatment options including prenylation inhibitors are awaiting clinical development for use in hepatitis D.
机译:D型肝炎是由D型肝炎病毒(HDV)感染引起的,被认为是人类病毒性肝炎中最严重的形式。丁型肝炎仅在HBV表面抗原(HBsAg)阳性的个体中发生,因为HDV是需要HBsAg传播的有缺陷的RNA病毒。已经描述了至少八种不同的HDV基因型,每种都有特征性的地理分布和独特的临床过程。 HDV和HBV合并感染可能与复杂和动态的病毒优势模式有关。慢性HDV感染比HBV单一感染导致更严重的肝脏疾病,并且与加速的纤维化进程,更早的肝代偿失调和肝细胞癌发展的风险增加有关。迄今为止,只有IFN-α疗法在人中证明对HDV具有抗病毒活性,并且与改善长期预后相关。在过去2年中进行的关于PEG-IFN-α使用的研究表明,以无法检测到的血清HDV RNA水平衡量,对治疗的持续病毒学应答可以在大约四分之一的D型肝炎患者中实现。包括戊酰化抑制剂在内的多种治疗选择正在等待D型肝炎的临床开发。

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