首页> 美国卫生研究院文献>Journal of Virology >The EBNA-2 arginine-glycine domain is critical but not essential for B-lymphocyte growth transformation; the rest of region 3 lacks essential interactive domains.
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The EBNA-2 arginine-glycine domain is critical but not essential for B-lymphocyte growth transformation; the rest of region 3 lacks essential interactive domains.

机译:EBNA-2精氨酸-甘氨酸结构域对于B淋巴细胞的生长转化至关重要但并非必不可少。区域3的其余部分缺少必要的交互域。

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摘要

Since deletion of region 3 (amino acids [aa] 333 to 425) of Epstein-Barr virus nuclear protein 2 (EBNA-2) results in EBV recombinants which cannot transform primary B lymphocytes (J. I. Cohen, F. Wang, and E. Kieff, J. Virol. 65:2545-2554, 1991), the role of domains of region 3 was investigated. Deletion of the Arg-Gly repeat domain, R-337GQSRGRGRGRGRGRGKG354, results in EBV recombinants that transform primary B lymphocytes with modestly decreased activity. The transformed cells grow slowly and are difficult to expand. EBNA-2 deleted for the Arg-Gly domain does not associate with the nuclear chromatin fraction. The Arg-Gly repeat has an intrinsic ability to bind to histone H1, to other proteins, including EBNA-1, and to nucleic acids, especially poly(G). Two independent deletions of each part of the rest of region 3 (aa 359 to 383 and 385 to 430) have little effect on transformation, while deletion of the rest of region 3 (aa 361 to 425) as a single segment substantially reduces transformation efficiency. EBNA-2 deleted for all of region 3 can still transactivate the LMP1 promoter in transient expression assays but is less active than EBNA-2 in transactivating the BamHI-C promoter. EBNA-2 deleted for the Arg-Gly domain is better than EBNA-2 at transactivating the LMP1 promoter and is as active as EBNA-2 in transactivating the BamHI-C promoter. These data are most compatible with a model in which the Arg-Gly domain of region 3 is a modulator of EBNA-2 interactions and activities, while the rest of region 3 is important in positioning the region 2 J kappa binding domain relative to the region 4 acidic transactivating domain. Despite the null phenotype of the region 3 deletion, region 3 is unlikely to mediate essential interactions with other proteins.
机译:由于爱泼斯坦-巴尔病毒核蛋白2(EBNA-2)的3区(氨基酸[aa] 333至425位)的缺失导致EBV重组体无法转化原代B淋巴细胞(JI Cohen,F。Wang和E. Kieff) ,J.Virol.65:2545-2554,1991),研究了区域3的结构域的作用。删除Arg-Gly重复结构域R-337GQSRGRGRGRGRGRGKGKG354,会导致EBV重组体转化原代B淋巴细胞,活性适度降低。转化的细胞生长缓慢且难以扩增。缺失的Arg-Gly结构域的EBNA-2与核染色质部分无关。 Arg-Gly重复序列具有与组蛋白H1,其他蛋白质(包括EBNA-1)以及核酸(尤其是poly(G))结合的固有能力。区域3其余部分(aa 359至383和385至430)的每个部分的两个独立删除对转化的影响很小,而区域3其余部分(aa 361至425)的缺失作为单个片段则大大降低了转化效率。在瞬时表达分析中,缺失了所有区域3的EBNA-2仍可以激活LMP1启动子,但在激活BamHI-C启动子方面比EBNA-2活性低。在反式激活LMP1启动子方面,缺失Arg-Gly结构域的EBNA-2优于EBNA-2,在反式激活BamHI-C启动子方面与EBNA-2一样有效。这些数据与其中区域3的Arg-Gly结构域是EBNA-2相互作用和活性的调节剂的模型最兼容,而区域3的其余部分在相对于区域定位区域2 Jκ结合域方面很重要。 4个酸性反式激活域。尽管区域3缺失的表型无效,区域3不太可能介导与其他蛋白质的必需相互作用。

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