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Protein sequence requirements for function of the human T-cell leukemia virus type 1 Rex nuclear export signal delineated by a novel in vivo randomization-selection assay.

机译:通过新型体内随机选择试验确定的1型人T细胞白血病病毒Rex核输出信号功能的蛋白质序列要求。

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The Rex protein of human T-cell leukemia virus type 1, like the functionally equivalent Rev protein of human immunodeficiency virus type 1, contains a leucine-rich activation domain that specifically interacts with the human nucleoporin-like Rab/hRIP cofactor. Here, this Rex sequence is shown to function also as a protein nuclear export signal (NES). Rex sequence libraries containing randomized forms of the activation domain/NES were screened for retention of the ability to bind Rab/hRIP by using the yeast two-hybrid assay. While the selected sequences differed widely in primary sequence, all were functional as Rex activation domains. In contrast, randomized sequences that failed to bind Rab/hRIP lacked Rex activity. The selected sequences included one with homology to the Rev activation domain/NES and a second that was similar to the NES found in the cellular protein kinase inhibitor alpha. A highly variant, yet fully active, activation domain sequence selected on the basis of Rab/hRIP binding retained full NES function even though this sequence preserved only a single leucine residue. In contrast, nonfunctional activation domain mutants that were unable to bind Rab/hRIP had also lost NES function. These data demonstrate that NES activity is a defining characteristic of the activation domains found in the Rev/Rex class of retroviral regulatory proteins and strongly support the hypothesis that the Rab/hRIP cofactor plays a critical role in mediating the biological activity of these NESs. In addition, these data suggest a consensus sequence for NESs of the Rev/Rex class.
机译:1型人类T细胞白血病病毒的Rex蛋白,与1型人类免疫缺陷病毒的功能等效的Rev蛋白一样,含有富含亮氨酸的激活域,该域与人核孔蛋白样Rab / hRIP辅因子特异性相互作用。在此,该Rex序列还显示出蛋白质核输出信号(NES)的功能。通过使用酵母双杂交测定法,筛选了包含随机形式的激活域/ NES的Rex序列文库,以保留结合Rab / hRIP的能力。虽然选择的序列在一级序列上有很大的不同,但所有序列都具有Rex激活域的功能。相反,未能结合Rab / hRIP的随机序列缺乏Rex活性。选择的序列包括一个与Rev激活域/ NES同源的序列,另一个类似于在细胞蛋白激酶抑制剂α中发现的NES。基于Rab / hRIP结合选择的高度变异但具有完全活性的激活域序列保留了完整的NES功能,即使该序列仅保留了一个亮氨酸残基。相比之下,无法结合Rab / hRIP的非功能性激活域突变体也失去了NES功能。这些数据表明,NES活性是逆转录病毒调节蛋白的Rev / Rex类中发现的激活域的定义特征,并强烈支持Rab / hRIP辅助因子在介导这些NES的生物学活性中起关键作用的假设。此外,这些数据表明了Rev / Rex类NES的共有序列。

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