| Literature DB >> 31175045 |
Dominik Hotter1, Matteo Bosso1, Kasper L Jønsson2, Christian Krapp3, Christina M Stürzel1, Atze Das4, Elisabeth Littwitz-Salomon5, Ben Berkhout4, Alina Russ6, Sabine Wittmann6, Thomas Gramberg6, Yue Zheng7, Laura J Martins7, Vicente Planelles7, Martin R Jakobsen2, Beatrice H Hahn8, Ulf Dittmer5, Daniel Sauter1, Frank Kirchhoff9.
Abstract
The interferon γ-inducible protein 16 (IFI16) is known as immune sensor of retroviral DNA intermediates. We show that IFI16 restricts HIV-1 independently of immune sensing by binding and inhibiting the host transcription factor Sp1 that drives viral gene expression. This antiretroviral activity and ability to bind Sp1 require the N-terminal pyrin domain and nuclear localization of IFI16, but not the HIN domains involved in DNA binding. Highly prevalent clade C HIV-1 strains are more resistant to IFI16 and less dependent on Sp1 than other HIV-1 subtypes. Furthermore, inhibition of Sp1 by IFI16 or pharmacologically by Mithramycin A suppresses reactivation of latent HIV-1 in CD4+ T cells. Finally, IFI16 also inhibits retrotransposition of LINE-1, known to engage Sp1, and murine IFI16 homologs restrict Friend retrovirus replication in mice. Thus, IFI16 restricts retroviruses and retrotransposons by interfering with Sp1-dependent gene expression, and evasion from this restriction may facilitate spread of HIV-1 subtype C.Entities:
Keywords: HIV-1; PYHIN proteins; Sp1 transcription factor; interferon γ-inducible PYHIN protein 16; restriction factors
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Year: 2019 PMID: 31175045 PMCID: PMC6681451 DOI: 10.1016/j.chom.2019.05.002
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023