HIV regulation of the IL-7R: a viral mechanism for enhancing HIV-1 replication in human macrophages in vitro

被引:13
|
作者
Zhang, Mingjie
Drenkow, Jorg
Lankford, Carla S. R.
Frucht, David M.
Rabin, Ronald L.
Gingeras, Thomas R.
Venkateshan, Chettemegre
Schwartzkopff, Franziska
Clouse, Kathleen A.
Dayton, Andrew I.
机构
[1] US FDA, Mol Virol Lab, Div Emerging & Transfus Transmitted Dis, Off Blood Res & Review,Ctr Biol Evaluat & Res,CBE, Rockville, MD 20852 USA
[2] US FDA, Lab Immunobiochem, DBPAP, Off Vaccine Res & Review,Ctr Biol Evaluat & Res, Rockville, MD 20852 USA
[3] Affymetrix, Santa Clara, CA USA
[4] Ctr Drug Evaluat & Res, Div Monoclonal Antibodies, Off Biotechnol Prod, Bethesda, MD USA
关键词
cytokine receptors; cytokines; Tat; AIDS;
D O I
10.1189/jlb.0704424
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
We report a novel mechanism, involving up-regulation of the interleukin (IL)-7 cytokine receptor, by which human immunodeficiency virus (HIV) enhances its own production in monocyte-derived macrophages (MDM) in vitro. HIV-1 infection or treatment of MDM cultures with exogenous HIV-1 Tat(86) protein up-regulates the IL-7 receptor (IL-7R) et-chain at the levels of steady-state RNA, protein, and functional IL-7R on the cell surface (as measured by ligand-induced receptor signaling). This IL-7R up-regulation is associated with increased amounts of HIV-1 virions in the supernatants of infected MDM cultures treated with exogenous IL-7 cytokine. The overall effect of IL-7 stimulation on HIV replication in MDM culture supernatants is typically in the range of one log and greater. The results are consistent with a model in which HIV infection produces the Tat protein, which in turn up-regulates IL-7R in a paracrine manner. This results in increased IL-7R signaling in response to the IL-7 cytokine, which ultimately promotes early events in HIV replication, including binding/entry and possibly other steps prior to reverse transcription. The results suggest that the effects of IL-7 on HIV replication in MDM should be considered when analyzing and designing clinical trials involving treatment of patients with IL-7 or Tat vaccines.
引用
收藏
页码:1328 / 1338
页数:11
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