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Herpes simplex virus UL56 interacts with and regulates the Nedd4-family ubiquitin ligase Itch

机译:单纯疱疹病毒UL56与Nedd4家族泛素连接酶Itch相互作用并对其进行调节

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Background Herpes simplex virus type 2 (HSV-2) is one of many viruses that exploits and modifies the cellular ubiquitin system. HSV-2 expresses the tegument protein UL56 that has been implicated in cytoplasmic transport and/or release of virions, and is a putative regulatory protein of Nedd4 ubiquitin ligase. In order to elucidate the biological function of UL56, this study examined the interaction of UL56 with the Nedd4-family ubiquitin ligase Itch and its role in the regulation of Itch. Additionally, we assessed the similarity between UL56 and regulatory proteins of Itch and Nedd4, Nedd4-family-interactins proteins (Ndfip). Results UL56 interacted with Itch, independent of additional viral proteins, and mediated more striking degradation of Itch, compared to Nedd4. Moreover, it was suggested that the lysosome pathway as well as the proteasome pathway was involved in the degradation of Itch. Other HSV-2 proteins with PY motifs, such as VP5 and VP16, did not mediate the degradation of endogenous Itch. Ndfip1 and Ndfip2 were similar in subcellular distribution patterns to UL56 and colocalized with UL56 in co-transfected cells. Conclusions We believe that this is the first report demonstrating the interaction of a HSV-specific protein and Itch. Thus, UL56 could function as a regulatory protein of Itch. The mechanism, function and significance of regulating Itch in HSV-2 infection remain unclear and warrant further investigation.
机译:背景2型单纯疱疹病毒(HSV-2)是许多利用和修饰细胞遍在蛋白系统的病毒之一。 HSV-2表达外皮蛋白UL56,该蛋白已与病毒体的胞质运输和/或释放有关,并且是Nedd4泛素连接酶的假定调控蛋白。为了阐明UL56的生物学功能,本研究检查了UL56与Nedd4家族泛素连接酶Itch的相互作用及其在Itch调节中的作用。此外,我们评估了UL56与Itch和Nedd4的调节蛋白,Nedd4家族相互作用素蛋白(Ndfip)之间的相似性。结果与Nedd4相比,UL56与Itch相互作用,独立于其他病毒蛋白,并介导了Itch的惊人降解。此外,建议溶酶体途径以及蛋白酶体途径都参与了Itch的降解。其他具有PY图案的HSV-2蛋白(例如VP5和VP16)不介导内源性Itch的降解。 Ndfip1和Ndfip2在亚细胞分布模式上与UL56相似,并且在共转染的细胞中与UL56共定位。结论我们认为这是第一份证明HSV特异性蛋白与Itch相互作用的报告。因此,UL56可以充当Itch的调节蛋白。在HSV-2感染中调节Itch的机制,功能和意义尚不清楚,有待进一步研究。

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