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建立并使用表达单纯疱疹病毒1型胸苷激酶的细胞系来鉴定病毒胸苷激酶依赖性耐药性。

Establishment and use of a cell line expressing HSV-1 thymidine kinase to characterize viral thymidine kinase-dependent drug-resistance.

作者信息

Kim Jee Hyun, Park Jong Beak, Bae Pan Kee, Kim Hae Soo, Kim Do Wan, Ahn Jeong Keun, Lee Chong-Kyo

机构信息

Pharmaceutical Screening Center, Korea Research Institute of Chemical Technology, Taejon 305-600, South Korea.

出版信息

Antiviral Res. 2002 Jun;54(3):163-74. doi: 10.1016/s0166-3542(01)00221-2.

Abstract

To understand the mechanisms of antiviral drug resistance and to have a system to examine the cytotoxicity of herpes simplex virus type 1 (HSV-1) inhibitors that are thymidine kinase (TK)-dependent, we have constructed a plasmid pFTK1 by inserting a DNA fragment containing the TK gene of HSV-1 strain F into the eukaryotic expression vector pcDNA3.1/His A. TK-deficient 143B cells were transfected with this vector and neomycin-resistant cells were selected. Cell survival in HAT medium and TK activity of the cell lysates were examined to ascertain HSV-1 TK expression. A cell line expressing the viral TK gene, FTK143B (FTK), was established and used for characterization of two laboratory-derived TK-deficient drug-resistant HSV-1 mutants of strain F. The antiviral activities of several drugs, mostly nucleoside analogues, were compared in the Vero, 143B and FTK cell culture systems. We showed that both mutant viruses lost their resistance to acyclovir and to other HSV-1 TK-dependent compounds in FTK cells but not in Vero and 143B cells. Significantly increased cytotoxicity of ganciclovir and (E)-5-(2-bromovinyl)-2'-deoxyuridine was also observed in the FTK cells. This HSV-1 TK gene-transfected cell model is a useful tool to rapidly determine HSV-1 drug resistance at the viral TK level.

摘要

为了解抗病毒药物耐药性的机制,并建立一个系统来检测依赖胸苷激酶(TK)的单纯疱疹病毒1型(HSV-1)抑制剂的细胞毒性,我们通过将包含HSV-1 F株TK基因的DNA片段插入真核表达载体pcDNA3.1/His A中,构建了质粒pFTK1。用该载体转染TK缺陷的143B细胞,并筛选出对新霉素耐药的细胞。检测细胞在HAT培养基中的存活率和细胞裂解物的TK活性,以确定HSV-1 TK的表达。建立了一个表达病毒TK基因的细胞系FTK143B(FTK),并用于对F株的两个实验室衍生的TK缺陷型耐药HSV-1突变体进行特性分析。在Vero、143B和FTK细胞培养系统中比较了几种药物(主要是核苷类似物)的抗病毒活性。我们发现,两种突变病毒在FTK细胞中对阿昔洛韦和其他依赖HSV-1 TK的化合物失去了耐药性,但在Vero和143B细胞中没有。在FTK细胞中还观察到更昔洛韦和(E)-5-(2-溴乙烯基)-2'-脱氧尿苷的细胞毒性显著增加。这种转染了HSV-1 TK基因的细胞模型是在病毒TK水平快速确定HSV-1耐药性的有用工具。

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