Sears A E, Meignier B, Roizman B
J Virol. 1985 Aug;55(2):410-6. doi: 10.1128/JVI.55.2.410-416.1985.
Herpes simplex virus 1 recombinants carrying alpha-, beta-, and late gamma (gamma 2)-regulated thymidine kinase (TK) genes were tested for the ability to establish latency in BALB/c mice inoculated by the eye route. The significant findings were as follows. Representatives of alpha- and gamma 2-regulated TK recombinants all established and maintained latent infections, but the efficiency was somewhat lower than that of wild-type virus. Of the three alpha TK recombinants tested, one (R316) spontaneously deleted portions of the inserted sequences which conferred alpha regulation to the TK gene. The viruses carrying these deletions expressed considerably lower TK activity than did wild-type virus, i.e., 2 to 40% of the levels expressed by the wild-type virus carrying the beta TK gene. However, the ability of these viruses to establish latency was not related to the efficiency of expression of the TK gene. These results indicate the following: (i) conversion of the TK gene into an alpha or gamma 2 gene did not preclude the establishment of latent infections; (ii) there was no correlation between the levels of TK activity expressed in cell culture and the ability to establish latency; and (iii) rearrangement of the genome by insertions or deletions which interrupt gene domains did not automatically result in an inability to establish latent infections.
携带α、β和晚期γ(γ2)调控的胸苷激酶(TK)基因的单纯疱疹病毒1重组体,经眼内接种BALB/c小鼠,测试其建立潜伏感染的能力。主要研究结果如下:α和γ2调控的TK重组体的代表株均能建立并维持潜伏感染,但效率略低于野生型病毒。在测试的三个α TK重组体中,一个(R316)自发缺失了赋予TK基因α调控的插入序列的部分片段。携带这些缺失的病毒表达的TK活性比野生型病毒低得多,即仅为携带β TK基因的野生型病毒所表达水平的2%至40%。然而,这些病毒建立潜伏感染的能力与TK基因的表达效率无关。这些结果表明:(i)将TK基因转化为α或γ2基因并不妨碍潜伏感染的建立;(ii)细胞培养中表达的TK活性水平与建立潜伏感染的能力之间没有相关性;(iii)通过插入或缺失导致基因结构域中断的基因组重排不会自动导致无法建立潜伏感染。
