Regad T, Saib A, Lallemand-Breitenbach V, Pandolfi P P, de Thé H, Chelbi-Alix M K
CNRS UPR 9051, Hôpital St Louis, 1 avenue Claude Vellefaux, 75475 Paris Cedex 10, France.
EMBO J. 2001 Jul 2;20(13):3495-505. doi: 10.1093/emboj/20.13.3495.
The promyelocytic leukaemia (PML) protein localizes in the nucleus both in the nucleoplasm and in matrix-associated multiprotein complexes known as nuclear bodies (NBs). The number and the intensity of PML NBs increase in response to interferon (IFN). Overexpression of PML affects the replication of vesicular stomatitis virus and influenza virus. However, PML has a less powerful antiviral activity against these viruses than the IFN mediator MxA. Here, we show that overexpression of PML, but not that of Mx1 or MxA, leads to a drastic decrease of a complex retrovirus, the human foamy virus (HFV), gene expression. PML represses HFV transcription by complexing the HFV transactivator, Tas, preventing its direct binding to viral DNA. This physical interaction requires the N-terminal region of Tas and the RING finger of PML, but does not necessitate PML localization in NBs. Finally, we show that IFN treatment inhibits HFV replication in wild-type but not in PML-/- cells. These findings point to a role for PML in transcriptional repression and suggest that PML could play a key role in mediating an IFN-induced antiviral state against a complex retrovirus.
早幼粒细胞白血病(PML)蛋白定位于细胞核内的核质以及与基质相关的多蛋白复合物中,这些复合物被称为核小体(NBs)。核小体的数量和强度会因干扰素(IFN)而增加。PML的过表达会影响水疱性口炎病毒和流感病毒的复制。然而,与IFN介质Mx A相比,PML对这些病毒的抗病毒活性较弱。在此,我们表明,PML的过表达而非Mx1或Mx A的过表达会导致复杂逆转录病毒——人类泡沫病毒(HFV)的基因表达大幅下降。PML通过与HFV反式激活因子Tas结合,阻止其直接与病毒DNA结合,从而抑制HFV转录。这种物理相互作用需要Tas的N端区域和PML的环指结构,但并不要求PML定位于核小体中。最后,我们表明IFN处理可抑制野生型细胞而非PML基因敲除细胞中的HFV复制。这些发现表明PML在转录抑制中发挥作用,并提示PML可能在介导IFN诱导的针对复杂逆转录病毒的抗病毒状态中起关键作用。