几种重要的信号转导通路.ppt

1、Major Developmental signaling pathways1.RTK Pathways:FGF,EGF,Jak-Stat 2.TGF-beta3.Wnt4.Hh5.Notch 6.10 Structure and function of a receptor tyrosine kinase6.12 The widely used RTK signal transduction pathway6.13 Activation of the Mitf transcription factor through the binding of stem cell factor by th

2、e Kit RTK protein(Part 2)Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.4 Ligand-induced dimerization of HER1,a human receptor for epidermal growth factor(EGF).Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.F

3、igure 16.5 Structure of the fibroblast growth factor(FGF)receptor,stabilized by heparan sulfate.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.6 Activation of EGF receptor by EGF results in the formation of an asymmetric kinase domain dimer.Copyrigh

4、t 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.7 The HER family of receptors and their ligands.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.8 Erythropoietin and formation of red blood cells(erythrocytes).

5、6.14 A STAT pathway:the casein gene activation pathway activated by prolactin Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.27 Structure of TGF-b b superfamily of signaling molecules.6.21 Relationships among members of the TGF-superfamily6.21 Relat

6、ionships among members of the TGF-superfamily(Part 1)6.21 Relationships among members of the TGF-superfamily(Part 2)6.23 The Smad pathway activated by TGF-superfamily ligands(Part 1)6.23 The Smad pathway activated by TGF-superfamily ligands(Part 2)Copyright 2013 by W.H.Freeman and CompanyMolecular C

7、ell Biology,7th EditionLodish et al.Figure 16.29 Model of Ski-mediated down-regulation of Smad transcription-activating function.Genetic control of Drosophila embryogenesis Edward B.Lewis Christiane Nuesslein-Volhard Eric Wieschaus Wg:GreenHh:RedSegment Polarity mutantswingless(wg)hedgehog(hh)Copyri

8、ght 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.30 Wnt signaling pathway.6.20 The Wnt signal transduction pathways(Part 1)6.20 The Wnt signal transduction pathways(Part 2)6.20 The Wnt signal transduction pathways(Part 3)Copyright 2013 by W.H.Freeman and Co

9、mpanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.31 Processing of Hedgehog(Hh)precursor protein.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.32 Hedgehog signaling in flies.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biolog

10、y,7th EditionLodish et al.Figure 16.33 Hedgehog signaling in vertebrates.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish et al.Figure 16.34(a)Activation of the NF-B signaling pathway.Copyright 2013 by W.H.Freeman and CompanyMolecular Cell Biology,7th EditionLodish e

11、t al.Figure 16.34(b)Activation of the NF-B signaling pathway.6.26 Mechanism of Notch activityFigure 16.35 Notch/Delta signaling pathway.Figure 16.36 Proteolytic cleavage of APP and Alzheimers disease.Figure 16.40 Multiple signal transduction pathways interact to regulate adipocyte differentiation.Fi

12、gure 15.6 GTPase switch proteins cycle between active and inactive forms.Figure 15.7 Switching mechanism of G proteins.Figure 15.15 General structure of G proteincoupled receptors.Figure 15.17 General mechanism of the activation of effector proteins associated with G proteincoupled receptors.Experim

13、ental Figure 15.18 Activation of G proteins occurs within seconds of ligand binding in amoeba cells.Figure 15.20 Activation of the muscarinic acetylcholine receptor and its effector K+channel in heart muscle.Figure 15.32 Activation of CREB transcription factor following ligand binding to Gs proteinc

14、oupled receptors.Figure 15.34 Role of b b-arrestin in GPCR desensitization and signal transduction.Phenotypes of Mutants in the Wingless Sigaling Pathway Wild Type Loss of Wg Signaling Constitutive Wg SignalingWildtypewinglesssulfateless(sfl)sugarless(sgl)Phenotypes of sulfateless and sugarless Bios

15、ynthesis of Heparan Sulfate ProteoglycanH2COHCOOH2COHH2COHH2COHHNAcUDP-D-glucoseUDP-D-glucuronic acidUDP-D-glucose dehydrogenaseSugarless HS N-deacetylase/N-sulfotransferasesulfatelessUronosyl C5-epimerization2-O-sulfation6-O-sulfationCOOCOOCOOH2COHHNAcHNAcHNAcH2COHH2COHH2COHH2COHCOOCOOCOOCOOHNSO3HN

16、SO3HNSO3HNAcH2COSO3H2COSO3H2COSO3H2COHHNSO3HNSO3HNAcHNSO3Syndecan Glypican PerlecanStructure of Heparan Sulfate ProteoglycansThe Gal-4/UAS techniqueEnhancer Trap-Gal4UAS-Gene XXTranscriptional Activation of Gene XTussue Specific Expression of Gal-4UAS Genomic EnhancerBrand and Perrimon:Development(1

17、993)Gene XActivated Arm protein can rescue the cuticle defects of sfl and sgl Control PrdGAL4/UAS ArmActsflsglOverexpression of Wg in sfl and sgl can rescue Wg signaling defect in a dose dependent mannerControl16CPrd GAL4/UAS Wg 25CsflsglPrd GAL4/UAS WgDFZ2DFZ2HSPGWg expressing cellDFZ2DFZ2HSPGWg ex

18、pressing cellWild typesgl or sfl mutantsnGlypican in Wnt signaling nHaecker et al(1997)DevelopmentnLin and Perrimon(1999)Nature nLin et al(2001)Development nHan et al(2004)DevelopmentnHan et al(2005)Development nTao et al.(2005)CellnYan et al.(2009)Dev Cell nCK-1a in Wnt signaling nLiu,et al (2002)C

19、ellnPygopus(Pygo)in Wnt signaling:nBelenkaya et al(2002)Development nSchwab et al(2007)BMC BiologynSong et al(2007)Development Wnt信号通路成员的鉴定信号通路成员的鉴定2024/5/21 周二53Morphogen(形态发生素形态发生素):An important concept in BiologyTuring,1952Morgan,1897Target genes Cell fates54发育过程中关键的形态发生素发育过程中关键的形态发生素nWnt/Wingles

20、snHedgehog(Hh)nTGF-/BMPnFGF特性特性1.进化上保守进化上保守2.对胚胎发育至关重要对胚胎发育至关重要3.功能异常与多种人类疾病密切相关功能异常与多种人类疾病密切相关2024/5/21 周二55Cell proliferation and differentiation.(Driesch 1891,1908)When he separated two sea urchin blastomeres,they produced twohalf-sized blastula,showing that cells are potentially independent,but

21、function together to form a whole organism(Driesch 1891,1908).(Morgan 1901).Morgan noted the polarity of organisms and that regeneration inworms occurs with different rates at different positions.This ledhim to postulate that regeneration phenomena are influenced bygradients of“formative substances”

22、Morphogen 56Morphogen“A form generating substance that diffuses through a tissue,its distribution dictating the development of cells in the tissue”Alan Turing(1952).The chemical basis of morphogenesis.Philos.Trans.R.Soc.Lond.B Biol.Sci.237,37-7257Growth Factor MorphogensSignaling molecules produced

23、in a restricted regions within a tissue.Morphogens emanate from their source to form a long-range concentration gradient.Receiving cells interpret morphogen gradient by activating target gene expression at discrete concentration thresholds thereby acquiring positional information.Two criteria:1.Conc

24、entration dependence.2.Direct action at a distanceWnt,Hh,and TGF-are morphogens.58形态发生素功能失调相关的人类疾病形态发生素功能失调相关的人类疾病前脑无裂畸形前脑无裂畸形(HPE)(HPE)骨发育不良骨发育不良神经管发育缺陷神经管发育缺陷肾母细胞瘤肾母细胞瘤 结肠癌结肠癌 家族性渗出性玻璃家族性渗出性玻璃体视网膜病变体视网膜病变 骨质疏松骨质疏松-假性神经胶质瘤假性神经胶质瘤综合症综合症(OPS)(OPS)裂足症裂足症先天性四肢切断症先天性四肢切断症2024/5/21 周二59Vertebrates:SHh Wn

25、t BMPHh,Wg,Dpp:essential morphogens in wing disc60 Key questions for morphogen gradient formation(1)how do they secreted (2)how do they move(3)how do they establish their activity gradients61Models for morphogen MovementTwo main modelsDiffusionTranscytosisOther modelsCytonemesArgosomes62Dpp is a mor

26、phogen in wing patterning Dpp Sal Omb P-MADUAS-GFP-Dpp Dpp-Gal463Models on Dpp movement A prevailing view is that Dpp moves across cells by planar transcytosis initiated by dynamin-mediated endocytosis.(Entchev,E.V.,Schwabedissen,A.,and Gonzalez-Gaitan,M.(2000).Cell 103,981-991)However,mathematical

27、modeling suggested that diffusive mechanism(s)is much more plausible than non-diffusive mechanisms.(Lander,A.D.,Nie,Q.,and Wan,F.Y.(2002).Dev Cell 2,785-796)Question:Which mechanism controls Dpp movement?64Extracellular Dpp gradient coincides with Dpp activity gradient in wing disc65Dynamin-mediated

28、 endocytosis66Dpp signaling is reduced cell-autonomously in dynamin-defective cells,but is normal in cells behind the dynamin-defective cells67Extracellular Dpp can move through dynamin-defective cells68Extracellular Dpp can move through dynamin-defective cells69Dynamin-mediated endocytosisIs requir

29、ed for Dpp signalingDown-regulates extracellular Dpp levelsIs not essential for Dpp movement70Structure of heparan sulfate proteoglycansSyndecanGlypicanPerlecanGene Number in Drosophila 12Dally Dally-like 17172Dpp fails to move across cells mutant for sflsfl mutant clones73Dpp fails to move across c

30、ells mutant for or dally-dlydally-dly mutant clones74Dpp fails to move across cells mutant for sfl or dally-dlyGFP-Dpp Extracellular Dpp Mergesfl dally-dly75The extracellular Dpp gradient represents Dpp activity gradient.Dynamin-mediated endocytosis is not required for Dpp movement,but is involved i

31、n Dpp signaling.The HSPGs Dally and Dly are required for Dpp movement.We propose that Dpp moves along the cell surface by attachment to the HSPGs Dally and Dly.76A model for Dpp movement across cells77形态发生素形态发生素（Wnt、Hh、BMP）梯度形成机制梯度形成机制限制扩散机制限制扩散机制Wnt morpohgen:Beag et al.(2001)Development Han et al.

32、2004)Development.Han et al.(2005)Development Tao et al.(2005)Cell Yan et al(2009)Developmental Cell Hh morphogen:Han et al (2004)Development Yan et al(2010)Development BMP morphogen:Belenkaya et al(2004)Cell78Wg acts as a morphogen in the wing discDllSensMergeExtracellular Wg 79Wnt Secretion Model

33、in 2006 Wntless/Evi/SrtK.Balser lab(2006)CellM.Boutros lab(2006)CellE.Selva Lab(2007)Development 80What is Retromer complex?81What does retromer do?821.Retrieval of receptors from endosomes to Golgi-Lysosomal hydrolases in mammalian cells-Vacuolar hydrolases in yeast2.Promoting of polymeric immunogl

34、obulin receptor transcytosisKnown functions of retromer complex83Role of retrormer complex in Wingless signalingPrevious views:Retromer is required for Wnt signaling.Retromer controls Wnt signaling in its producing cells.Disruption of retromer affects Wnt gradient formationRetromer may control Wnt m

35、odifications or association with lipoproteins.Coudreuse et al.Science,2006;Prasad et al.Development,2006.Questions:How does retromer control Wnt signaling activity in Wnt producing cells?84Generation of dVps35 null mutant and RNAi construct85Wg is accumulated in dVps35 mutant cellsdVps35 clonesUAS-d

36、Vps35 Ri/En-G486Depletion of dVps35 decreases Wg secretion in S2 cells87Retromer is not required for Hh and Dpp functionsHh distribution and signaling Dpp signaling 88In the absence of dVps35 activity:Wg protein is accumulated inside Wg-producing cells,but reduced on the cell surface of Wg-producing

37、 cells and in surrounding Wg-recieving cells.Wg protein levels are reduced in conditioned medium.Conclusion:Retromer is required for Wg secretion.Question:How Does Retromer regulate Wg secretion?89Similarity between dvps35 and Wls mutantsBAWgGFPE-cadmergeBAWgGFPE-cadmergeBAWgGFPE-cadmergeBAWgGFPE-ca

38、dmergeGFP Wg MergewlsHypothesis:Retromer may control Wg/Wnt secretion by regulating Wls activity90dVps35 interacts with Wls91Question:What would happen with Wls in the absence of retromer?92Wls GFP Merge Wls protein is reduced in the vps35 mutant cells 93Retromer controls Wls stability6hrs8hrsWls-V5

39、 Hh-G4/vps35 RNAi Wls-V5 Hh-G4/vps35 RNAi1hr3hrs94QuestionsWhat is the cellular distribution of Wls?What is the role of retromer in regulating Wls activity?95Wls is distributed on the cell surface 96Localization of Wls on cell membraneWls-V5CD8-mRFPmerge97Wls particles co-localize with endosome mark

40、ersRab5-GFP Wls Merge GFP-2xFYVE Wls Merge 98Dynamin-mediated endocytosis99Wls is elevated on the plasma membrane of shi cellsshits1Rab5(RNAi)hrsd28Wls DE-cad Merge 100Dynamin-mediated endocytosis101Enhanced Wls levels in rab5 and hrs mutantshrs cloneWls Rab5 MergeRab5 RNAiHh-Gal4Wls DE-cad Merge 10

41、2Question:Does Retromer regulate Wnt secretion using similar mechanism(s)in vertebrate cells?103Depletion of Vps35 reduced Wnt3A and Wnt5A secretion104hWls forms a complex with Vps35105Human retromer complex controls the stability of hWls protein 106Belenkaya et al.Developmental Cell 2008 Port et al

42、Nature Cell Biology 2008Yang et al.Developmental Cell 2008 Franch-Marro et al.Nature Cell Biology 2008Pan et al.Developmental Cell 2008Wnt Secretion Model in 2008107Question 1:Whats role of retromer in Wnt signalingQuestion 2:Mechanisms of Retrmer in Wnt secretion:Role of Snx3 in Wnt secretionQuest

43、ion 3:Roles of Retromer in other developmental patterning:Apical-Basal Polarity108 What does Retromer do?109Homology between Human sorting nexins and Drosophila SNXs110 Null allels of Drosophila SNX homologues111Generation of Dsnx3 Null mutants by P-element hopping 112Dsnx3 is required for Wg secret

44、ion and signaling113 Wg expression monitored by wg-lacZ is not alteredExtracellular Wg is reduced in the Dsnx3 mutant cells 114Wg(conditioned media)Wg(lysate)Beta-actinControl RNAi1 RNAi2 Dsnx3 is essential for Wg secretion in cultured S2 cells115Dsnx3 is required for Wg secretion and signalingUAS-D

45、snx12RNAi116Dsnx3 function is not essential for Hh and Dpp signaling117 HypothesisDsnx3 influences Wnt secretion by disrupting Wls recycling from endosomes to the Trans-Golgi Network.118Wls levels were markedly reduced in Dsnx3 clones Wg secretion defect can be rescued by Wls overexpression 119 Dsnx

46、3 can colocalize with hWls in early Endosomes of Hela cells 120Dsnx3 interacts with Dwls in S2 cells121 Mutiple alignment of Snx3 homologue genes PtdIns3P binding motif 122PtdIns3P binding site is essential for Dsnx3 functionUAS-SNX12-EGFPMerge 123 Dsnx3Wnt Secretion model in 2011124Casali&Batlle,20

47、09,Cell Stem Cell 4:124-127.哺乳动物结肠隐窝哺乳动物结肠隐窝果蝇中肠果蝇中肠ISC:Intestinal Stem Cells ISC:Intestinal Stem Cells 肠干细胞肠干细胞TA:Transient Amplifying TA:Transient Amplifying 短暂扩充细胞短暂扩充细胞EB:Enteroblast cells EB:Enteroblast cells 成肠细胞成肠细胞EC:Eterocyte cells EC:Eterocyte cells 肠上皮细胞肠上皮细胞EE:Enteroendocrine cells EE:En

48、teroendocrine cells 内分泌细胞内分泌细胞果蝇中肠是研究果蝇中肠是研究稳态（稳态（homeostasis)维持和维持和干细胞调控干细胞调控的理想系统的理想系统 关键科学问题：关键科学问题：形态发生素信号如何调控干细胞和组织稳态维持？形态发生素信号如何调控干细胞和组织稳态维持？2024/5/21 周二125BMPBMP信号通过气管与肠道两种不同器官之间的对话来实现信号通过气管与肠道两种不同器官之间的对话来实现调控肠道干细胞和组织内稳态调控肠道干细胞和组织内稳态Li et al.,Developmental Cell 2013Highlighted by F1000BMPBMP信

49、号通过气管与肠道两种不同器官之信号通过气管与肠道两种不同器官之间的对话来实现调控肠道干细胞和组织内间的对话来实现调控肠道干细胞和组织内稳态；提出器官稳态；提出器官-器官之间建立信号通讯器官之间建立信号通讯并协同调控稳态维持的概念并协同调控稳态维持的概念126HhHh信号调控肠干细胞活性和稳态维持信号调控肠干细胞活性和稳态维持Li et al.,Li et al.,Stem Cell Reports 2014Stem Cell Reports 2014HhHh信号通过激活信号通过激活JNKJNK和和JAK/STATJAK/STAT调调控稳态维持控稳态维持127Zorn AM and Wells JM.Annu.Rev.Cell Cev Biol.2009哺乳动物内胚层器官的形成及谱系建立哺乳动物内胚层器官的形成及谱系建立2024/5/21 周二128Model of early A-P patterningMesodermEndodermZorn and Wells(2009)Annu Rev Cell Dev Biol.Wnt signaling and endoderm patterning?repress foregut identity promote hindgut fate2024/5/21 周二129