Sinha-Datta Uma, Datta Abhik, Ghorbel Sofiane, Dodon Madeleine Duc, Nicot Christophe
Department of Microbiology, University of Kansas Medical Center, Kansas City, KS 66160, USA.
J Biol Chem. 2007 May 11;282(19):14608-15. doi: 10.1074/jbc.M611219200. Epub 2007 Mar 14.
Human T-cell lymphotrophic virus type I Rex and p30 are both RNA binding regulatory proteins. Rex is a protein that interacts with a responsive element and stimulates nuclear export of incompletely spliced viral RNAs thereby increasing production of virus particles. In contrast, p30 is involved in the nuclear retention of the tax/rex mRNA leading to inhibition of virus expression and possible establishment of viral latency. How these two proteins, with apparent opposite functions, integrate in the viral replication cycle is unknown. Here, we demonstrate that Rex and p30 form ribonucleoprotein ternary complexes onto specific viral mRNA. Our results explain the selective nuclear retention of tax/rex but not other viral mRNAs by p30. Whereas p30 suppresses Rex expression, it did not affect Rex-mediated nuclear export of RNA containing the Rex response element. In contrast, Rex was able to counteract p30-mediated suppression of viral expression and restore cytoplasmic tax/rex mRNA and Tax protein expression. Together, our data demonstrate a complex regulatory mechanism of antagonizing post-transcriptional regulators evolved by human T-cell lymphotrophic virus type I to allow a vigilant control of viral gene expression.
人类I型嗜T细胞淋巴细胞病毒(HTLV-I)的Rex蛋白和p30蛋白都是RNA结合调节蛋白。Rex蛋白是一种与反应元件相互作用并刺激不完全剪接的病毒RNA核输出的蛋白质,从而增加病毒颗粒的产生。相比之下,p30参与tax/rex mRNA的核滞留,导致病毒表达受到抑制并可能建立病毒潜伏状态。这两种功能明显相反的蛋白质如何在病毒复制周期中整合尚不清楚。在此,我们证明Rex蛋白和p30蛋白在特定的病毒mRNA上形成核糖核蛋白三元复合物。我们的结果解释了p30对tax/rex而非其他病毒mRNA的选择性核滞留。虽然p30抑制Rex蛋白的表达,但它不影响Rex介导的含有Rex反应元件的RNA的核输出。相反,Rex蛋白能够抵消p30介导的病毒表达抑制,并恢复细胞质中tax/rex mRNA和Tax蛋白的表达。总之,我们的数据证明了人类I型嗜T细胞淋巴细胞病毒进化出的一种对抗转录后调节因子的复杂调节机制,以实现对病毒基因表达的精确控制。
