Arya S K
Laboratory of Tumor Cell Biology, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892.
AIDS Res Hum Retroviruses. 1991 Dec;7(12):1007-14. doi: 10.1089/aid.1991.7.1007.
Human immunodeficiency virus type 2 (HIV-2) gene expression is downmodulated by sequence elements downstream of the transcriptional initiation site, corresponding to the U5 region of the long terminal repeat (LTR) and further downstream. This repression appeared to be related more to the length of the sequence intervening the transcriptional initiation site and the coding region than to a particular sequence content. The repressive effect of the downstream segment was not affected by HIV-2 and HIV-1 TAT or by the cytomegalovirus transactivator IE-2 gene. Nor was it affected by T-cell activation signals or by such cytokines as tumor necrosis factor-alpha (TNF-alpha), interleukin-6 (IL-6), interferon-gamma (IFN gamma), and interferon-alpha (IFN alpha). In contrast to HIV-1, HIV-2 LTR-directed gene expression was not modulated by TNF-alpha. A specific sequence element, located downstream of the TAR element in the R region, seemed to participate in modulation of gene expression. This element interacted with a nuclear protein with a mobility of about 26 kD. The repressive effect of the downstream sequence was to a certain extent cell type dependent, suggesting the involvement of cell type-specific factors. It was more effective in human lymphocytic CEM cells than in Jurkat cells. This may be relevant to the HIV-2 cell tropism (replication), latency, and virulence.
2型人类免疫缺陷病毒(HIV-2)的基因表达受到转录起始位点下游序列元件的下调,这些元件对应于长末端重复序列(LTR)的U5区域及更下游区域。这种抑制作用似乎更多地与转录起始位点和编码区域之间的序列长度有关,而非特定的序列内容。下游片段的抑制作用不受HIV-2和HIV-1反式激活因子TAT或巨细胞病毒反式激活因子IE-2基因的影响。它也不受T细胞激活信号或肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)、干扰素-γ(IFNγ)和干扰素-α(IFNα)等细胞因子的影响。与HIV-1不同,HIV-2 LTR指导的基因表达不受TNF-α的调节。位于R区域TAR元件下游的一个特定序列元件似乎参与了基因表达的调节。该元件与一种迁移率约为26 kD的核蛋白相互作用。下游序列的抑制作用在一定程度上依赖于细胞类型,提示细胞类型特异性因子的参与。它在人淋巴细胞CEM细胞中比在Jurkat细胞中更有效。这可能与HIV-2的细胞嗜性(复制)、潜伏性和毒力有关。
