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标题: 原发性人肝细胞乙型肝炎病毒X蛋白的时空分析 [打印本页]

作者: StephenW    时间: 2019-7-31 09:12     标题: 原发性人肝细胞乙型肝炎病毒X蛋白的时空分析

Spatiotemporal Analysis of Hepatitis B Virus X Protein in Primary Human Hepatocytes
Dmytro Kornyeyev, Dhivya Ramakrishnan, Christian Voitenleitner, Christine M. Livingston, Weimei Xing, Magdeleine Hung, Hyock Joo Kwon, Simon P. Fletcher, Rudolf K. Beran
J.-H. James Ou, Editor
DOI: 10.1128/JVI.00248-19

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ABSTRACT

The structural maintenance of chromosomes 5/6 complex (Smc5/6) is a host restriction factor that suppresses hepatitis B virus (HBV) transcription. HBV counters this restriction by expressing the X protein (HBx), which redirects the host DNA damage-binding protein 1 (DDB1) E3 ubiquitin ligase to target Smc5/6 for degradation. HBx is an attractive therapeutic target for the treatment of chronic hepatitis B (CHB), but it is challenging to study this important viral protein in the context of natural infection due to the lack of a highly specific and sensitive HBx antibody. In this study, we developed a novel monoclonal antibody that enables detection of HBx protein in HBV-infected primary human hepatocytes (PHH) by Western blotting and immunofluorescence. Confocal imaging studies with this antibody demonstrated that HBx is predominantly located in the nucleus of HBV-infected PHH, where it exhibits a diffuse staining pattern. In contrast, a DDB1-binding-deficient HBx mutant was detected in both the cytoplasm and nucleus, suggesting that the DDB1 interaction plays an important role in the nuclear localization of HBx. Our study also revealed that HBx is expressed early after infection and has a short half-life (∼3 h) in HBV-infected PHH. In addition, we found that treatment with small interfering RNAs (siRNAs) that target DDB1 or HBx mRNA decreased HBx protein levels and led to the reappearance of Smc6 in the nuclei of HBV-infected PHH. Collectively, these studies provide the first spatiotemporal analysis of HBx in a natural infection system and also suggest that HBV transcriptional silencing by Smc5/6 can be restored by therapeutic targeting of HBx.

IMPORTANCE Hepatitis B virus X protein (HBx) is a promising drug target since it promotes the degradation of the host structural maintenance of chromosomes 5/6 complex (Smc5/6) that inhibits HBV transcription. To date, it has not been possible to study HBx in physiologically relevant cell culture systems due to the lack of a highly specific and selective HBx antibody. In this study, we developed a novel monoclonal HBx antibody and performed a spatiotemporal analysis of HBx in a natural infection system. This revealed that HBx localizes to the nucleus of infected cells, is expressed shortly after infection, and has a short half-life. In addition, we demonstrated that inhibiting HBx expression or function promotes the reappearance of Smc6 in the nucleus of infected cells. These data provide new insights into HBx and underscore its potential as a novel target for the treatment of chronic HBV infection.
作者: StephenW    时间: 2019-7-31 09:13

原发性人肝细胞乙型肝炎病毒X蛋白的时空分析
Dmytro Kornyeyev,Dhivya Ramakrishnan,Christian Voitenleitner,Christine M. Livingston,Weimei Xing,Magdeleine Hung,Hyock Joo Kwon,Simon P. Fletcher,Rudolf K. Beran
J.-H. James Ou,编辑
DOI:10.1128 / JVI.00248-19

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抽象

染色体5/6复合物(Smc5 / 6)的结构维持是抑制乙型肝炎病毒(HBV)转录的宿主限制因子。 HBV通过表达X蛋白(HBx)来抵抗这种限制,该蛋白将宿主DNA损伤结合蛋白1(DDB1)E3泛素连接酶重定向至目标Smc5 / 6以进行降解。 HBx是治疗慢性乙型肝炎(CHB)的有吸引力的治疗靶点,但由于缺乏高度特异性和敏感性的HBx抗体,在自然感染的背景下研究这种重要的病毒蛋白具有挑战性。在这项研究中,我们开发了一种新型单克隆抗体,通过蛋白质印迹和免疫荧光检测HBV感染的原代人肝细胞(PHH)中的HBx蛋白。使用该抗体的共聚焦成像研究证明HBx主要位于HBV感染的PHH的细胞核中,其中它表现出弥散染色模式。相反,在细胞质和细胞核中均检测到DDB1结合缺陷的HBx突变体,表明DDB1相互作用在HBx的核定位中起重要作用。我们的研究还表明,HBx在感染后早期表达,并且在HBV感染的PHH中具有短半衰期(约3小时)。此外,我们发现用靶向DDB1或HBx mRNA的小干扰RNA(siRNA)处理降低了HBx蛋白水平并导致Smc6再次出现在HBV感染的PHH的细胞核中。总的来说,这些研究提供了自然感染系统中HBx的第一次时空分析,并且还表明通过治疗性靶向HBx可以恢复Smc5 / 6的HBV转录沉默。

重要性乙型肝炎病毒X蛋白(HBx)是一种很有前途的药物靶点,因为它可以促进抑制HBV转录的染色体5/6复合物(Smc5 / 6)的宿主结构维持的降解。迄今为止,由于缺乏高度特异性和选择性的HBx抗体,尚无法在生理学相关的细胞培养系统中研究HBx。在这项研究中,我们开发了一种新的单克隆HBx抗体,并在自然感染系统中对HBx进行了时空分析。这表明HBx定位于感染细胞的细胞核,在感染后不久表达,并且半衰期短。此外,我们证明抑制HBx表达或功能促进Smc6在感染细胞的细胞核中再现。这些数据为HBx提供了新的见解,并强调了其作为治疗慢性HBV感染的新靶点的潜力。
作者: StephenW    时间: 2019-7-31 09:16

https://jvi.asm.org/content/jvi/93/16/e00248-19.full.pdf




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