1. Small Molecule Inhibition of HIV-1–Induced MHC-I Down-Regulation Identifies a Temporally Regulated Switch in Nef Action
- Author
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Matthew D. Wortman, Ben Kukull, Masateru Hiyoshi, Danielle M. Williamson, Angela M. Gronenborn, Gary Thomas, Masafumi Takiguchi, Katelyn M. Atkins, Jinwon Jung, Hirokazu Koizumi, In Ja L. Byeon, Lori A. Emert-Sedlak, Eric Barklis, Laurel Thomas, Jimmy D. Dikeakos, Jinwoo Ahn, Thomas E. Smithgall, Shinya Suzu, and Masumichi Saito
- Subjects
CD4-Positive T-Lymphocytes ,Time Factors ,Vesicular Transport Proteins ,Down-Regulation ,chemical and pharmacologic phenomena ,Plasma protein binding ,Phosphatidylinositol 3-Kinases ,Endocytosis ,Cell Line ,Small Molecule Libraries ,03 medical and health sciences ,0302 clinical medicine ,Multienzyme Complexes ,MHC class I ,Humans ,nef Gene Products, Human Immunodeficiency Virus ,Src family kinase ,Molecular Biology ,030304 developmental biology ,0303 health sciences ,biology ,Histocompatibility Antigens Class I ,PTEN Phosphohydrolase ,virus diseases ,Articles ,Cell Biology ,Molecular biology ,Small molecule ,3. Good health ,Cell biology ,Transport protein ,Transcription Factor AP-1 ,Protein Transport ,src-Family Kinases ,Cell Biology of Disease ,HIV-1 ,biology.protein ,Signal transduction ,030217 neurology & neurosurgery ,Protein Binding ,Signal Transduction - Abstract
Nef assembles a multi-kinase complex triggering MHC-I down-regulation. We identify an inhibitor that blocks MHC-I down-regulation, identifying a temporally regulated switch in Nef action from directing MHC-I endocytosis to blocking cell surface delivery. These findings challenge current dogma and reveal a regulated immune evasion program., HIV-1 Nef triggers down-regulation of cell-surface MHC-I by assembling a Src family kinase (SFK)-ZAP-70/Syk-PI3K cascade. Here, we report that chemical disruption of the Nef-SFK interaction with the small molecule inhibitor 2c blocks assembly of the multi-kinase complex and represses HIV-1–mediated MHC-I down-regulation in primary CD4+ T-cells. 2c did not interfere with the PACS-2–dependent trafficking of Nef required for the Nef-SFK interaction or the AP-1 and PACS-1–dependent sequestering of internalized MHC-I, suggesting the inhibitor specifically interfered with the Nef-SFK interaction required for triggering MHC-I down-regulation. Transport studies revealed Nef directs a highly regulated program to down-regulate MHC-I in primary CD4+ T-cells. During the first two days after infection, Nef assembles the 2c-sensitive multi-kinase complex to trigger down-regulation of cell-surface MHC-I. By three days postinfection Nef switches to a stoichiometric mode that prevents surface delivery of newly synthesized MHC-I. Pharmacologic inhibition of the multi-kinase cascade prevents the Nef-dependent block in MHC-I transport, suggesting the signaling and stoichiometric modes are causally linked. Together, these studies resolve the seemingly controversial models that describe Nef-induced MHC-I down-regulation and provide new insights into the mechanism of Nef action.
- Published
- 2010
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