HIV发病机理.pptx
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1、HIVCellular Pathogenesis IIBenhur Lee,M.D.HIV Accessory Genes:TatRevVifVprVpuNefEssential in vitro and in vivoEssential in certain cell types(Permissive vs Non-permissive cells)Non-essential in vitro,but leads to attenuated phenotype in vivo Tat:Transactivator of HIVs LTR PromoterExperimental Observ
2、ations:Binding of Tat to TAR in vitro does NOT require loop sequences known to be necessary in vivo for functionPre-incubation of nuclear extracts with recombinant Tat depletes a factor necessary for Tat-mediated transcription in vitroTat functions poorly in rodent cells unless complemented by facto
3、r(s)present on Chromosome 12(radiation hybrids)Tat associates with a kinase complex that hyperphosphorylates CTD of RNAP II(identified thru an in vitro drug screen for Tat inhibitors)-this kinase is Cdk9,but Cdk9 does NOT bind Tat!?Mystery human-specific co-factor for Tat activity must exist2 struct
4、ure of HIV TAR sequence“loop”“bulge”Predicted and confirmed properties of Tat co-factor:Cyclin TBinds directly to Tat in a complex with Cdk9Increases the affinity of Tat for TARIncreases the specificity of Tat for“loop”and“bulge”residuesTat-CycT-Cdk9 complex hyperphosphorylates CTD of RNAP II and in
5、creases HIV transcriptional processivityCycT maps to chromosome 12,and potentiates Tat trans-activation in murine cells 50-to 100-foldMurine homolog of human CycT does NOT bind to TatTat:Transactivator of HIVs LTR PromoterExperimental Observations Explained:Binding of Tat to TAR in vitro does NOT re
6、quire loop sequences known to be necessary in vivo for functionPre-incubation of nuclear extracts with recombinant Tat depletes a factor necessary for Tat-mediated transcription in vitroTat functions poorly in rodent cells unless complemented by factor(s)present on Chromosome 12(radiation hybrids)Ta
7、t associates with a kinase complex that hyperphosphorylates CTD of RNAP II(identified thru an in vitro drug screen for Tat inhibitors)-this kinase is Cdk9,but Cdk9 does NOT bind Tat!?Mystery human-specific co-factor for Tat activity must exist:Cyclin TRevEssential for nuclear export of unspliced or
8、single spliced viral transcriptsImportin-b bRanGDPArg Rich Domain(ARD)-binds to Importin-b b for nuclear import After nuclear import,Ran-GDP is convertedto Ran-GTP,and importin-b b dissociates from Rev“Free”ARD now can bind to RRE,but only in context of Rev multimersRevNuclear Export Signal(NES),leu
9、cine-rich domain,binds Exportin-1(XPO)cooperatively with Ran-GTPRevRevImportin-b bRan-GDPRcc1Ran-GTPRan-GDPRan-GTPRanGAPImportin-b bRanGTPNefMajor determinant of pathogenicity in vivonef-deleted SIV is severely attenuated in the rhesus macaque model infection of macaques with recombinant SIV carryin
10、g a premature STOP codon(point mutation)results in rapid revertants with the nef ORF Patients infected with nef-defective HIV have a dramatically decreased rate of disease progression(15 years)nef-deleted HIV do not deplete thymocytes as much,or replicate to as high titers,as wild-type HIV in the SC
11、ID-hu mice modelPleiotropic Functions of NefN-myristoylation required for Nef activity-implies that membranelocalization of nef is critical for its activityMGxxx(S/T)(K/R)(K/R)MGxxx(S)(K)(K/R)100%100%99%50%ConsensusN-myristoylationSignal:HIV sequenceConservation inNef protein:Pleiotropic Functions o
12、f NefDown-regulates cell surface levels of CD4Down-regulates surface levels of major histocompatibility class I moleculesMediates cellular signaling and activation Enhances viral infectivity I.Down-modulation of surface CD4Down-modulation of surface CD4 via internalization followed by degradation vi
13、a endosomal/lysosomal pathway Advantages:Prevents disadvantageous super-infection of host cellEnhance viral progeny release(by preventing Env-mediated sequestration of CD4 in secretory pathway)Evidence:Nef expression increases number of CD4 containing clathrin-coated pitsNef-induced CD4 down-modulat
14、ion blocked by inhibitors of clathrin-coated pit-mediated endocytosis (e.g.ikaguramycin)Inhibition of lysosomal acidification(e.g.via chloroqine treatment)blocks Nef-induced CD4 degradationExpression of nef alone in T-cell lines can lead to CD4 downregulation(as determined by FACS)CD4Nef-GFP.I.Down-
15、modulation of surface CD4Mechanism(s)?Direct interaction with CD4 has not been biochemically demonstrable,but NMR analysis suggest a direct interaction with Kd 0.87 m mM;yeast two-hybrid assays also suggest an interactionActs as a connector to the host-cell endocytic machineryCo-localizes with AP-2
16、on inner plasma membraneConserved dileucine based sorting motif(E/DxxxL)in Nef is important for both CD4-down-modulation and AP-2 co-localizationInteracts with NBP-1(identified through a yeast two-hybrid screen).NBP-1 is part of the vacuolar membrane ATPase complex in clathrin-coated pits(H subunit
17、of vacuolar ATPase-VH1)C-terminal diacidic motif(DD)in Nef is important for NBP-1 interaction,and,at least in SIV Nef,the dileucine motif is also important for NBP-1 interactions?May bind to b b-Cop,a coatamer protein which targets proteins to lysosomesNBP-1II.Down-modulation of MHC Class IAdvantage
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- HIV 发病 机理
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