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重组干扰素-γ对乙型肝炎病毒DNA复制中间形式的抑制作用

Inhibition of hepatitis B virus DNA replicative intermediate forms by recombinant interferon-gamma.

作者信息

Parvez Mohammad-Khalid, Sehgal Deepak, Sarin Shiv-Kumar, Basir Seemi-Farhat, Jameel Shahid

机构信息

Department of Biosciences, Jamia Millia Islamia, New Delhi, Virology Group, International Centre for Genetic Engineering and Biotechnology, New Delhi, India.

出版信息

World J Gastroenterol. 2006 May 21;12(19):3006-14. doi: 10.3748/wjg.v12.i19.3006.

DOI:10.3748/wjg.v12.i19.3006
PMID:16718779
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4124373/
Abstract

AIM

To evaluate the in vitro anti-HBV activity of recombinant human IFN-gamma, alone and in combination with lamivudine.

METHODS

A recombinant baculovirus-HBV/HepG2 culture system was developed which could support productive HBV infection in vitro. Expression of HBsAg and HBeAg in infected HepG2 culture medium was detected by commercial enzyme immunoassays. HBV DNA replication intermediates were detected in infected cells by Southern hybridization and viral DNA load was determined by dot hybridization.

RESULTS

IFN-gamma at 0.1 to 5 microg/L efficiently down regulated HBsAg expression in transduced HepG2 cells. At 5 microg/L, IFN-gamma also suppressed HBV DNA replication in these cells. While treatment with a combination of lamivudine and IFN-gamma showed no additive effect, sequential treatment first with lamivudine and then IFN-gamma was found to be promising. In this culture system the best HBV suppression was observed with a pulse of 2 micromol/L lamivudine for two days, followed by 1 microg/L IFN-gamma for another four days. Compared to treatment with lamivudine alone, the sequential use of 0.2 micromol/L lamivudine for two days, followed by 5 microg/L IFN-gamma for six days showed a 72% reduction in HBV cccDNA pool.

CONCLUSION

This in vitro study warrants further evaluation of a combination of IFN-gamma and lamivudine, especially in IFN-alpha non-responder chronic hepatitis B patients. A reduced duration of lamivudine treatment would also restrict the emergence of drug-resistant HBV mutants.

摘要

目的

评估重组人干扰素-γ单独及与拉米夫定联合使用时的体外抗乙肝病毒活性。

方法

构建了一种重组杆状病毒-乙肝病毒/ HepG2培养系统,该系统可支持乙肝病毒在体外的有效感染。通过商业酶免疫测定法检测感染的HepG2培养基中HBsAg和HBeAg的表达。通过Southern杂交检测感染细胞中的乙肝病毒DNA复制中间体,并通过点杂交确定病毒DNA载量。

结果

0.1至5μg/L的干扰素-γ可有效下调转导的HepG2细胞中HBsAg的表达。在5μg/L时,干扰素-γ也可抑制这些细胞中的乙肝病毒DNA复制。虽然拉米夫定和干扰素-γ联合治疗未显示出相加作用,但发现先使用拉米夫定再使用干扰素-γ的序贯治疗很有前景。在该培养系统中,观察到最佳的乙肝病毒抑制效果是先用2μmol/L拉米夫定脉冲处理两天,然后用1μg/L干扰素-γ再处理四天。与单独使用拉米夫定治疗相比,先使用两天0.2μmol/L拉米夫定,然后使用六天5μg/L干扰素-γ的序贯治疗使乙肝病毒cccDNA池减少了72%。

结论

这项体外研究值得进一步评估干扰素-γ和拉米夫定的联合使用,尤其是在对干扰素-α无反应的慢性乙型肝炎患者中。缩短拉米夫定治疗时间也将限制耐药乙肝病毒突变体的出现。

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