Gibbs J S, Lackner A A, Lang S M, Simon M A, Sehgal P K, Daniel M D, Desrosiers R C
New England Regional Primate Research Center, Harvard Medical School, Southborough, Massachusetts 01772-9102.
J Virol. 1995 Apr;69(4):2378-83. doi: 10.1128/JVI.69.4.2378-2383.1995.
Rhesus monkeys (Macaca mulatta) were experimentally infected with strains of simian immunodeficiency virus (SIV) derived from SIVmac239 lacking vpr, vpx, or both vpr and vpx genes. These auxiliary genes are not required for virus replication in cultured cells but are consistently conserved within the SIVmac/human immunodeficiency virus type 2/SIVsm group of primate lentiviruses. All four rhesus monkeys infected with the vpr deletion mutant showed an early spike in plasma antigenemia, maintained high virus burdens, exhibited declines in CD4+ lymphocyte concentrations, and had significant changes in lymph node morphology, and two have died to date with AIDS. The behavior of the vpr deletion mutant was indistinguishable from that of the parental, wild-type virus. Rhesus monkeys infected with the vpx deletion mutant showed lower levels of plasma antigenemia, lower virus burdens, and delayed declines in CD4+ lymphocyte concentrations but nonetheless progressed with AIDS to a terminal stage. The vpr+vpx double mutant was severely attenuated, with much lower virus burdens and no evidence of disease progression. These and other results indicate that vpr provides only a slight facilitating advantage for wild-type SIVmac replication in vivo. Thus, progression to AIDS and death can occur in the absence of a gene for vpr or vpx.
恒河猴(猕猴)被用源自SIVmac239且缺失vpr、vpx或同时缺失vpr和vpx基因的猿猴免疫缺陷病毒(SIV)毒株进行实验性感染。这些辅助基因在培养细胞中并非病毒复制所必需,但在灵长类慢病毒的SIVmac/人类免疫缺陷病毒2型/SIVsm组中一直保持保守。所有四只感染vpr缺失突变体的恒河猴均出现血浆抗原血症早期峰值,维持高病毒载量,CD4 +淋巴细胞浓度下降,淋巴结形态有显著变化,且已有两只死于艾滋病。vpr缺失突变体的行为与亲本野生型病毒无异。感染vpx缺失突变体的恒河猴血浆抗原血症水平较低,病毒载量较低,CD4 +淋巴细胞浓度下降延迟,但仍进展至艾滋病终末期。vpr + vpx双突变体严重减毒,病毒载量低得多,且无疾病进展迹象。这些及其他结果表明,vpr仅为野生型SIVmac在体内的复制提供轻微的促进优势。因此,在没有vpr或vpx基因的情况下也可发生进展至艾滋病和死亡。
