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    請使用永久網址來引用或連結此文件: https://irlib.pccu.edu.tw/handle/987654321/35383


    題名: Cellular Nuclear Export Factors TAP and Aly Are Required for HDAg-L-mediated Assembly of Hepatitis Delta Virus
    作者: Huang, HC (Huang, Hsiu-Chen)
    Lee, CP (Lee, Chung-Pei)
    Liu, HK (Liu, Hui-Kang)
    Chang, MF (Chang, Ming-Fu)
    Lai, YH (Lai, Yu-Heng)
    Lee, YC (Lee, Yu-Ching)
    Huang, C (Huang, Cheng)
    貢獻者: 化學系
    關鍵詞: MESSENGER-RNA EXPORT
    FRAGMENT-LENGTH-POLYMORPHISM
    HUMAN PRIMARY HEPATOCYTES
    SIGNAL-INTERACTING PROTEIN
    B SURFACE-ANTIGEN
    LARGE FORM
    REPLICATION
    DOMAIN
    IDENTIFICATION
    TRANSPORT
    日期: 2016-12-09
    上傳時間: 2017-02-10 14:15:21 (UTC+8)
    摘要: Hepatitis delta virus (HDV) is a satellite virus of hepatitis B virus (HBV). HDV genome encodes two forms of hepatitis delta antigen (HDAg), small HDAg (HDAg-S), which is required for viral replication, and large HDAg (HDAg-L), which is essential for viral assembly. HDAg-L is identical to HDAg-S except that it bears a 19-amino acid extension at the C terminus. Both HDAgs contain a nuclear localization signal (NLS), but only HDAg-L contains a CRM1-independent nuclear export signal at its C terminus. The nuclear export activity of HDAg-L is important for HDV particle formation. However, the mechanisms of HDAg-L-mediated nuclear export of HDV ribonucleoprotein are not clear. In this study, the host cellular RNA export complex TAP-Aly was found to form a complex with HDAg-L, but not with an export-defective HDAg-Lmutant, in which Pro(205) was replaced by Ala. HDAg-L was found to colocalize with TAP and Aly in the nucleus. The C-terminal domain of HDAg-L was shown to directly interact with the N terminus of TAP, whereas an HDAg-L mutant lacking the NLS failed to interact with full-length TAP. In addition, small hairpin RNA-mediated down-regulation of TAP or Aly reduced nuclear export of HDAg-L and assembly of HDV virions. Furthermore, a peptide, TAT-HDAg-L(198-210), containing the 10-amino acid TAT peptide and HDAg-L(198-210), inhibited the interaction between HDAg-L and TAP and blocked HDV virion assembly and secretion. These data demonstrate that formation and release of HDV particles are mediated by TAP and Aly.
    關聯: JOURNAL OF BIOLOGICAL CHEMISTRY 卷: 291 期: 50 頁碼:26226-26238
    顯示於類別:[化學系所] 期刊論文

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