入胞抑制剂Myrcludex-B合成肽对HBV感染HepaRG细胞体外感染模型的抑制作用研究

目的建立乙型肝炎病毒(HBV)阳性血清体外感染人肝癌细胞(HepaRG)的实验模型,并探索入胞抑制剂Myrcludex-B在体外感染模型中对HBV的抑制作用。方法将诱导成熟的HepaRG细胞分成加聚乙二醇(PEG)的感染组和无PEG的感染组,再将两种感染组分别分为添加Myrcludex-B肽段的处理组和不添加Myrcludex-B肽段的对照组,用HBV DNA阳性患者的血清对细胞进行感染。取细胞上清液,用荧光定量PCR检测上清液中HBV DNA的表达量,用化学荧光法检测细胞上清液中HBsAg、HBeAg的含量。两组间计量资料不服从正态分布的采用秩和检验,服从正态分布的采用t检验,以P<0.05为差异有统计学意义。结果在处理组中,加PEG感染组和不加PEG感染组的病毒滴度分别为(103877.00±49013.24)拷贝/ml、(5050.09±631.26)拷贝/ml;在对照组中,加PEG感染组和不加PEG感染组的病毒滴度分别为(116188.57±50957.19)拷贝/ml、(5119.34±1102.43)拷贝/ml,两组中加PEG感染组的病毒滴度显著高于不加PEG感染组(P<0.05),差异有统计学意义。在加PEG的感染组中,加肽段处理组和无肽段对照组的病毒滴度分别为(103877.34±49013.24)拷贝/ml、(116188.57±50957.19)拷贝/ml,加肽段处理组病毒滴度明显下降(P<0.05),差异有统计学意义;该组0、1、2、3 d上清液中HBsAg的含量均为阳性,且0 d上清液中加肽段处理组的HBsAg较无肽段对照组呈明显下降趋势。结论用添加PEG的HBV DNA阳性血清体外感染HepaRG细胞的实验模型是可行的,且在该试验模型中,入胞抑制剂Myrcludex-B对HBV感染存在一定的抑制作用。

An update on the management of chronic hepatitis D

Hepatitis D virus(HDV)infection is associated with severe liver-related morbidity and mortality.The prevalence of HDV is rising especially among people who abuse drugs and immigrants from endemic areas.Reliable diagnostic assays with enhanced sensitivity and specificity are essential for screening at-risk populations.Until recently,interferon has been the only treatment for hepatitis D.Its efficacy is,however,limited and it is associated with significant side effects.A number of novel antiviral agents that target various stages of the HDV life cycle show promising results.They are currently in different phases of clinical development.This review focuses on the changing epidemiology,novel therapeutic agents,and updated management of chronic hepatitis delta.