首页> 外文OA文献 >A Protein Encoded by the Herpes Simplex Virus (HSV) Type 1 2-Kilobase Latency-Associated Transcript Is Phosphorylated, Localized to the Nucleus, and Overcomes the Repression of Expression from Exogenous Promoters When Inserted into the Quiescent HSV Genome

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A Protein Encoded by the Herpes Simplex Virus (HSV) Type 1 2-Kilobase Latency-Associated Transcript Is Phosphorylated, Localized to the Nucleus, and Overcomes the Repression of Expression from Exogenous Promoters When Inserted into the Quiescent HSV Genome

机译：由单纯疱疹病毒（HSV）1型2-千碱基潜伏期相关转录本编码的蛋白质被磷酸化，定位于细胞核，并克服了插入到静态HSV基因组中外源启动子的表达抑制。

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Herpes simplex virus (HSV) is characterized by its ability to establish a latent infection in sensory neurons, from which it can periodically reactivate. The mechanisms of latency, however, remain unclear. The HSV genome is quiescent during latency except for the expression of the latency-associated transcripts (LATs). Although the exact function of the LATs remains obscure, current evidence suggests they are multifunctional and are involved in both establishment of latency and reactivation from latency. The LATs contain several open reading frames (ORFs). One or more of the functions of the LATs could therefore be protein mediated. We have previously reported that deregulated expression of the largest of the HSV type 1 (HSV-1) LAT ORFs (∼274 amino acids) greatly enhances virus growth in cell types that are normally relatively nonpermissive for HSV replication and also that it complements mutations to the immediate-early (IE) gene ICP0 (S. K. Thomas, G. Gough, D. S. Latchman, and R. S. Coffin, J. Virol. 73:6618-6625, 1999). Here we show that LAT ORF expression overcomes the repression of expression from exogenous promoters introduced into the HSV-1 genome which normally occurs in the absence of IE gene expression. To further explore LAT ORF function, we have generated an epitope-tagged LAT ORF, LATmycHis, which forms punctate structures in the infected-cell nucleus reminiscent of the structures formed by ICP0. These are associated with the appearance of a phosphorylated form of the protein and are formed adjacent to, or around the edges of, viral replication compartments. These results provide further evidence that the HSV-1 LAT ORF protein is biologically functional and that the tightly regulated expression of this protein may be important in the wild-type latency phenotype in vivo.

机译：单纯疱疹病毒（HSV）的特征是能够在感觉神经元中建立潜伏感染，并可以周期性地重新激活它。但是，延迟的机制仍不清楚。 HSV基因组在潜伏期中处于静止状态，除了潜伏期相关转录本（LAT）的表达外。尽管LAT的确切功能仍然不清楚，但是目前的证据表明它们是多功能的，并且参与建立潜伏期和从潜伏期重新激活。 LAT包含几个开放阅读框架（ORF）。因此，LAT的一种或多种功能可能是蛋白质介导的。我们之前曾报道过，最大的HSV 1型（HSV-1）LAT ORF（〜274个氨基酸）的失调表达大大增强了通常相对不允许HSV复制的细胞类型中的病毒生长，并且它补充了突变即早（IE）基因ICP0（SK Thomas，G.Gough，DS Latchman，and RS Coffin，J.Virol。73：6618-6625，1999）。在这里，我们表明，LAT ORF表达克服了导入HSV-1基因组的外源启动子对表达的抑制，该启动子通常在没有IE基因表达的情况下发生。为了进一步探索LAT ORF的功能，我们产生了一个表位标记的LAT ORF LATmycHis，它在感染细胞核中形成点状结构，让人联想到ICP0形成的结构。这些与蛋白质磷酸化形式的出现有关，并且在病毒复制区室附近或边缘附近形成。这些结果提供了进一步的证据，表明HSV-1 LAT ORF蛋白具有生物学功能，并且该蛋白的严格调控的表达在体内野生型潜伏表型中可能很重要。

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Thomas, S. K.; Lilley, C. E.; Latchman, D. S.; Coffin, R. S.;
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年度 2002
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专利

1. The herpes simplex virus type 1 (HSV-1) latency-associated transcript (LAT) protects cells against cold-shock-induced apoptosis by maintaining phosphorylation of protein kinase B (AKT) [J] . Carpenter Dale, Hsiang Chinhui, Jiang Xianzhi, Journal of neurovirology . 2015 ,第5期

机译：单纯疱疹病毒1型（HSV-1）潜伏期相关转录本（LAT）通过维持蛋白激酶B（AKT）的磷酸化保护细胞免受冷休克诱导的细胞凋亡
2. Decreased reactivation of a herpes simplex virus type 1 (HSV-1) latency-associated transcript (LAT) mutant using the in vivo mouse UV-B model of induced reactivation [J] . BenMohamed Lbachir, Osorio Nelson, Srivastava Ruchi, Journal of neurovirology . 2015 ,第5期

机译：使用体内小鼠UV-B诱导再激活模型降低单纯疱疹病毒1型（HSV-1）潜伏期相关转录本（LAT）突变体的重新激活
3. The latency-associated gene of herpes simplex virus type 1 (HSV-1) interferes with superinfection by HSV-1. [J] . Mador N, Panet A, Steiner I Journal of neurovirology . 2002 ,第Suppla2期

机译：单纯疱疹病毒1型（HSV-1）的潜伏期相关基因干扰HSV-1的过度感染。
4. The Restructuring of Glycoprotein D of Herpes Simplex Virus 1 (HSV-1) for Cytoreductive Therapy of Malignant Gliomas in Humans [C] . Zhou GY, Kamiyama H, Roizman B World Engineers' Convention 2004 vol B: Biological Engineering and Health Care; 20041102-06; Shanghai(CN) . 2004

机译：单纯疱疹病毒1（HSV-1）糖蛋白D的重组，用于人类恶性胶质瘤的细胞还原治疗。
5. Herpes simplex virus type I (HSV-1)-induced cell fusion: Influence of viral glycoprotein D alleles and cell surface expression of glycosaminoglycans on cell fusion mediated by HSV entry receptors HveA, HveB and HveC. [D] . Terry-Allison, Tracy Lynn. 1999

机译：I型单纯疱疹病毒（HSV-1）诱导的细胞融合：病毒糖蛋白D等位基因和糖胺聚糖的细胞表面表达对HSV进入受体HveA，HveB和HveC介导的细胞融合的影响。
6. A Protein Encoded by the Herpes Simplex Virus (HSV) Type 1 2-Kilobase Latency-Associated Transcript Is Phosphorylated Localized to the Nucleus and Overcomes the Repression of Expression from Exogenous Promoters When Inserted into the Quiescent HSV Genome [O] . S. K. Thomas, C. E. Lilley, D. S. Latchman, 2002

机译：由单纯疱疹病毒（HSV）1型2-千碱基潜伏期相关转录本编码的蛋白质被磷酸化定位于核并克服了插入到静态HSV基因组中外源启动子的表达抑制。
7. Herpes Simplex Virus Type 1 (HSV-1)-Induced Apoptosis in Human Dendritic Cells as a Result of Downregulation of Cellular FLICE-Inhibitory Protein and Reduced Expression of HSV-1 Antiapoptotic Latency-Associated Transcript Sequences▿ [O] . Kather, Angela, Raftery, Martin J., Devi-Rao, Gayathri, 2009

机译：单纯疱疹病毒1型（HSV-1）诱导的人树突状细胞凋亡是细胞FLICE抑制蛋白下调和HSV-1抗凋亡潜伏期相关转录序列表达降低的结果▿
8. Upstream Promoter Elements of the Herpes Simplex Virus Type 1 Glycoprotein H Gene [R] . Steffy, K. R., Weir, J. P. 1991

机译：单纯疱疹病毒1型糖蛋白H基因的上游启动子元件

A Protein Encoded by the Herpes Simplex Virus (HSV) Type 1 2-Kilobase Latency-Associated Transcript Is Phosphorylated, Localized to the Nucleus, and Overcomes the Repression of Expression from Exogenous Promoters When Inserted into the Quiescent HSV Genome

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