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Nef enhances c-Cbl phosphorylation in HIV-infected CD4+ T lymphocytes
Authors:Yang Polung  Henderson Andrew J
Institution:Integrated Bioscience Graduate Program in Immunobiology, Department of Veterinary Science, Immunology Research Laboratories, 115 Henning Building, Pennsylvania State University, University Park, PA 16802, USA
Abstract:The multifunctional HIV-1 protein Nef possesses several motifs that interact with signaling molecules in infected T cells. In order to determine whether Nef influences T cell activation, cells were infected with Nef-positive and Nef-negative clones of HIV. CD28 expression and changes in tyrosine phosphorylation were monitored. We observed no Nef-dependent changes in CD28 expression or function. However, infection with Nef-positive virus led to changes in tyrosine phosphorylation. This Nef-induced phosphorylation was observed in unstimulated cells, and c-Cbl was identified as one of the proteins whose phosphorylation was upregulated by Nef. Furthermore, Lck is required for Nef-mediated c-Cbl tyrosine phosphorylation. These results suggest that Nef modifies T cell signaling in the absence of T cell receptor engagement and co-stimulation.
Keywords:TCR  T cell receptor  HIV-1  human immunodeficiency virus type 1  LTR  long terminal repeat  CHO  Chinese hamster ovary  PBS  phosphate-buffered saline  BSA  bovine serum albumin  PI3K  phosphatidylinositol 3&prime  -kinase  PP1  4-amino-5-[4-methylphenyl]-7-[t-butyl]pyrazolo[3  4-d]pyrimidine  FBS  fetal bovine serum  FACS  fluorescence-activated cell sorting  MFI  mean fluorescence intensity  PLAP  placental alkaline phosphatase  CSF-1  colony-stimulating factor-1  PDGFR  platelet-derived growth factor receptor  EGFR  epidermal growth factor receptor  NFAT  nuclear factor of activated T cells  AP-1  activator protein 1  SH2  Src-homology 2  SH3  Src homology 3  NF-κB  nuclear factor κB  FITC  fluorescein isothiocyanate  GEF  guanine nucleotide exchange factor  PMA  phorbol myristate acetate
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