Ross T M, Narayan M, Fang Z Y, Minella A C, Green P L
Department of Microbiology and Immunology, Vanderbilt University School of Medicine, Nashville, Tennessee 37232-2363, USA.
J Virol. 2000 Mar;74(6):2655-62. doi: 10.1128/jvi.74.6.2655-2662.2000.
Human T-cell leukemia virus (HTLV) Tax protein has been implicated in the HTLV oncogenic process, primarily due to its pleiotropic effects on cellular genes involved in growth regulation and cell cycle control. To date, several approaches attempting to correlate Tax activation of the CREB/activating transcription factor (ATF) or NFkappaB/Rel transcriptional activation pathway to cellular transformation have yielded conflicting results. In this study, we use a unique HTLV-2 provirus (HTLV(c-enh)) that replicates by a Tax-independent mechanism to directly assess the role of Tax transactivation in HTLV-mediated T-lymphocyte transformation. A panel of well-characterized tax-2 mutations is utilized to correlate the respective roles of the CREB/ATF or NFkappaB/Rel signaling pathway. Our results demonstrate that viruses expressing tax-2 mutations that selectively abrogate NFkappaB/Rel or CREB/ATF activation display distinct phenotypes but ultimately fail to transform primary human T lymphocytes. One conclusion consistent with our results is that the activation of NFkappaB/Rel provides a critical proliferative signal early in the cellular transformation process, whereas CREB/ATF activation is required to promote the fully transformed state. However, complete understanding will require correlation of Tax domains important in cellular transformation to those Tax domains important in the modulation of gene transcription, cell cycle control, induction of DNA damage, and other undefined activities.
人类T细胞白血病病毒(HTLV)的Tax蛋白与HTLV的致癌过程有关,主要是因为它对参与生长调节和细胞周期控制的细胞基因具有多效性作用。迄今为止,几种试图将Tax对CREB/激活转录因子(ATF)或NFκB/Rel转录激活途径的激活与细胞转化相关联的方法得出了相互矛盾的结果。在本研究中,我们使用一种独特的HTLV-2前病毒(HTLV(c-enh)),其通过不依赖Tax的机制进行复制,以直接评估Tax反式激活在HTLV介导的T淋巴细胞转化中的作用。利用一组特征明确的tax-2突变来关联CREB/ATF或NFκB/Rel信号通路的各自作用。我们的结果表明,表达选择性消除NFκB/Rel或CREB/ATF激活的tax-2突变的病毒表现出不同的表型,但最终未能转化原代人T淋巴细胞。与我们的结果一致的一个结论是,NFκB/Rel的激活在细胞转化过程早期提供关键的增殖信号,而CREB/ATF激活是促进完全转化状态所必需的。然而,要完全理解这一过程,需要将在细胞转化中重要的Tax结构域与在基因转录调节、细胞周期控制、DNA损伤诱导及其他未明确活动中重要的Tax结构域相关联。