评价HIV-1抗病毒药物的重组假病毒法的建立及其初步应用

目的:探讨重组似病毒方法应用于评价抗病毒药物的可行性。方法:采用 pSG3△env/TZM-bl 系统,制备假病毒毒种,在不同细胞,不同重组假病毒接种量的条件下,血用重组假病毒法测定 AZT 的抗病毒效果,以此选择最适的细胞接种量、病毒接种量,砰价检测方法的重复性,用建立的假病毒检测法测定 AZT、3TC、d4T、ddI 的抗病毒效果。结果:细胞接种量对检测结果有一定的影响,最适细胞接种量为每孔10~4个细胞;重组假病毒接种量对检测结果没有明显的羞异;重复性检测结果显示,该方法的 RSD 为11.52%;用该法检测 AZT、3TC、d4T、ddI 的50%抑制浓度(IC_(50)值)分别为0.0074 μmol·L^(-1)、0.5312 μmol·L^(-1)、0.0868 μmol·L^(-1)、3.4364 μmol·L^(-1)。结论:重组假病毒法可用于评价抗 HIV-1约物,具有快速、简便的优点。

Novel approaches towards conquering hepatitis B virus infection

Currently approved treatments for hepatitis B virus （HBV） infection include the immunomodulatory agent, IFN-α, and nucleos（t）ide analogues. Their efficacy is limited by their side effects, as well as the induction of viral mutations that render them less potent. It is thus necessary to develop drugs that target additional viral antigens. Chemicals and biomaterials by unique methods of preventing HBV replication are currently being developed, including novel nucleosides and newly synthesized compounds such as capsid assembling and mRNA transcription inhibitors. Molecular therapies that target different stages of the HBV life cycle will aid current methods to manage chronic hepatitis B （CriB） infection. The use of immunomodulators and gene therapy are also under consideration. This report summarizes the most recent treatment possibilities for CHB infection. Emerging therapies and their potential mechanisms, efficacy, and pitfalls are discussed.