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Identification of the Nuclear Export and Adjacent Nuclear Localization Signals for ORF45 of Kaposis Sarcoma-Associated Herpesvirus

机译:卡波西氏肉瘤相关疱疹病毒ORF45的核出口和邻近核定位信号的鉴定。

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摘要

Open reading frame 45 (ORF45) of Kaposi's sarcoma-associated herpesvirus 8 (KSHV) is an immediate-early phosphorylated tegument protein and has been shown to play important roles at both early and late stages of viral infection. Homologues of ORF45 exist only in gammaherpesviruses, and their homology is limited. These homologues differ in their protein lengths and subcellular localizations. We and others have reported that KSHV ORF45 is localized predominantly in the cytoplasm, whereas its homologue in murine herpesvirus 68 is localized exclusively in the nucleus. We observed that ORF45s of rhesus rhadinovirus and herpesvirus saimiri are found exclusively in the nucleus. As a first step toward understanding the mechanism underlying the distinct intracellular distribution of KSHV ORF45, we identified the signals that control its subcellular localization. We found that KSHV ORF45 accumulated rapidly in the nucleus in the presence of leptomycin B, an inhibitor of CRM1 (exportin 1)-dependent nuclear export, suggesting that it could shuttle between the nucleus and cytoplasm. Mutational analysis revealed that KSHV ORF45 contains a CRM1-dependent, leucine-rich-like nuclear export signal and an adjacent nuclear localization signal. Replacement of the key residues with alanines in these motifs of ORF45 disrupts its shuttling between the cytoplasm and nucleus. The resulting ORF45 mutants have restricted subcellular localizations, being found exclusively either in the cytoplasm or in the nucleus. Recombinant viruses were reconstituted by introduction of these mutations into KSHV bacterial artificial chromosome BAC36. The resultant viruses have distinct phenotypes. A mutant virus in which ORF45 is restricted to the cytoplasm behaves as an ORF45-null mutant and produces 5- to 10-fold fewer progeny viruses than the wild type. In contrast, mutants in which the ORF45 protein is mostly restricted to the nucleus produce numbers of progeny viruses similar to those produced by the wild type. These data suggest that the subcellular localization signals of ORF45 have important functional roles in KSHV lytic replication.
机译:卡波西氏肉瘤相关疱疹病毒8(KSHV)的开放阅读框45(ORF45)是一种立即早期磷酸化的外皮蛋白,已显示在病毒感染的早期和晚期均起重要作用。 ORF45的同源物仅存在于伽玛疱疹病毒中,并且它们的同源性受到限制。这些同源物的蛋白长度和亚细胞定位不同。我们和其他人已经报道,KSHV ORF45主要定位在细胞质中,而它在鼠疱疹病毒68中的同源物仅定位在细胞核中。我们观察到,恒河猴鼠鼻病毒和疱疹病毒赛米尔的ORF45仅在细胞核中发现。作为了解KSHV ORF45独特细胞内分布基础机制的第一步,我们鉴定了控制其亚细胞定位的信号。我们发现KSHV ORF45在瘦素B(一种依赖CRM1(出口蛋白1)的依赖型核出口的抑制剂)的存在下在核中迅速积累,表明它可以在核和细胞质之间穿梭。突变分析表明,KSHV ORF45包含依赖CRM1的富含亮氨酸的核输出信号和相邻的核定位信号。在ORF45的这些基序中,用丙氨酸取代关键残基会破坏其在细胞质和细胞核之间的穿梭。所得的ORF45突变体具有受限的亚细胞定位,仅在细胞质或细胞核中发现。通过将这些突变引入KSHV细菌人工染色体BAC36中来重组重组病毒。所得病毒具有不同的表型。 ORF45被限制在细胞质中的突变病毒表现为ORF45无效突变体,其后代病毒的数量比野生型少5至10倍。相反,ORF45蛋白主要限于细胞核的突变体产生的后代病毒数量与野生型病毒相似。这些数据表明ORF45的亚细胞定位信号在KSHV裂解复制中具有重要的功能作用。

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