免疫球蛋白的结构与功能的关系PPT讲稿.ppt
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1、免疫球蛋白的结构与功能的关系第1页,共52页,编辑于2022年,星期五Signalling antigen receptors on B cells-bifunctional antigen-binding secreted molecules(B 细胞表面受体和分泌的抗体)Structural conservation and infinite variability-domain structure(结构上不仅保守而且无限可变的).The Immunoglobulin Gene Superfamily(免疫球蛋白的超家族)The immunoglobulin fold(免疫球蛋白的折叠)F
2、ramework and complementarity determining regions-hypervariable loops(框架结构和可变区)Modes of interactions with antigens(与抗原相互作用的模型)Effector mechanisms and isotype role of the Fc.(Fc 区的作用)Multimeric antibodies and multimerisationCharacteristics and properties of each Ig isotypeIg receptors and their functi
3、onsImmunoglobulin Structure-Function Relationship第2页,共52页,编辑于2022年,星期五Cell surface antigen receptor on B cells B 细胞表面受体和分泌的抗体Allows B cells to sense their antigenic environmentConnects extracellular space with intracellular signalling machinerySecreted antibody(抗体)Neutralisation(中和作用)Arming/recruiti
4、ng effector cells(激活或者诱导功能细胞)Complement fixation(帮助机体对抗原的清除)Immunoglobulin Structure-Function Relationship第3页,共52页,编辑于2022年,星期五Immunoglobulins are Bifunctional ProteinsImmunoglobulins must interact with a small number of specialised molecules-(免疫球蛋白必须与特殊分子相互作用)Fc receptors on cells(细胞表面的Fc受体)Complem
5、ent proteins(辅助蛋白)Intracellular cell signalling molecules(细胞内信号转导分子)whilst simultaneously recognising an infinite array of antigenic determinants.(同时能够识别无限抗原族)第4页,共52页,编辑于2022年,星期五Structural conservation and a capacity for infinite variability in a single molecule is provided by a DOMAIN structure.(
6、结构上不仅保守而且无限可变的-抗体结构域)Ig domains are derived from a single ancestral gene that has duplicated,diversified and been modified to endow an assortment of functional qualities on a common basic structure(Ig结构域源于一个原始基因,复制,多元化,修饰等)Ig domains are not restricted to immunoglobulins(Ig 结构域不仅仅局限于免疫球蛋白).The most
7、striking characteristic of the Ig domain is a disulphide bond-linked structure of 110 amino acids long(Ig结构域最明显的特点是其双硫键,连接了110个氨基酸).Immunoglobulin domains第5页,共52页,编辑于2022年,星期五The genes encoding Ig domains are not restricted to Ig genes.Although first discovered in immunoglobulins,they are found in a
8、 superfamily of related genes,particularly those encoding proteins crucial to cell-cell interactions and molecular recognition systems.IgSF molecules are found in most cell types and are present across taxonomic boundariesIg gene superfamily-IgSF第6页,共52页,编辑于2022年,星期五Antibodies are Proteins that Reco
9、gnize Specific Antigens 抗体能够特异性的识别抗原抗体能够特异性的识别抗原第7页,共52页,编辑于2022年,星期五Epitopes(抗原决定簇(抗原决定簇):Antigen Regions that Interact with Antibodies第8页,共52页,编辑于2022年,星期五Consequences of Antibody Binding抗体结合效应抗体结合效应第9页,共52页,编辑于2022年,星期五CLVLSSSSSSSSCH3CH2CH1VHFcFabF(ab)2Domains are folded,compact,protease resistan
10、t structuresDomain Structure of Immunoglobulins免疫球蛋白的结构域免疫球蛋白的结构域Pepsin cleavage sites -1 x(Fab)2&1 x FcPapain cleavage sites -2 x Fab 1 x FcLight chain Cdomainsk or lHeavy chain Cdomainsa,d,e,g,or m第10页,共52页,编辑于2022年,星期五CH3第11页,共52页,编辑于2022年,星期五CH3CH2第12页,共52页,编辑于2022年,星期五CH3CH2CH1第13页,共52页,编辑于2022
11、年,星期五CH3CH2CH1VH1第14页,共52页,编辑于2022年,星期五CH3CH2CH1VH1VL第15页,共52页,编辑于2022年,星期五CH3CH2CH1VH1CLVL第16页,共52页,编辑于2022年,星期五CH3CH2CH1VH1CLVL第17页,共52页,编辑于2022年,星期五HingeCH3CH2CH1VH1VLCLElbow第18页,共52页,编辑于2022年,星期五CH3CH2FbFvFvFvFbFvHingeElbowCH3CH2FbFvFlexibility andmotion of immunoglobulins第19页,共52页,编辑于2022年,星期五H
12、ingeFvFbFabCH3CH2CH1VH1VLCLFcElbowCarbohydrate第20页,共52页,编辑于2022年,星期五The Immunoglobulin FoldThe characteristic structural motif of all Ig domainsBarrel under constructionA barrel made of a sheet of staves arranged in a folded over sheetA b barrel of 7(CL)or 8(VL)polypeptide strands connected by loops
13、 and arranged to enclose a hydrophobic interiorSingle VL domain第21页,共52页,编辑于2022年,星期五Unfolded VL region showing 8 antiparallel b-pleated sheets connected by loops.NH2COOHS SThe Immunoglobulin Fold第22页,共52页,编辑于2022年,星期五Immunoglobulins must interact with a finite number of specialised molecules-Easily
14、 explained by a common Fc region irrespective of specificity-whilst simultaneously recognising an infinite array of antigenic determinants.In immunoglobulins,what is the structural basis for the infinite diversity needed to match the antigenic universe?Immunoglobulins are Bifunctional Proteins第23页,共
15、52页,编辑于2022年,星期五Amino acid No.Variability8010060402020406080100120Cytochromes CVariability of amino acids in related proteinsWu&Kabat 1970Amino acid No.Variability8010060402020406080100120HumanIg heavychains第24页,共52页,编辑于2022年,星期五FR1FR2FR3FR4CDR2CDR3CDR1Distinct regions of high variability and conser
16、vation led to the concept of a FRAMEWORK(FR),on which hypervariable regions were suspended.Framework and Hypervariable regionsAmino acid No.Variability8010060402020406080100120Most hypervariable regions coincided with antigen contact points-the COMPLEMENTARITY DETERMINING REGIONS(CDRs)第25页,共52页,编辑于2
17、022年,星期五Hypervariable regionsHypervariable CDRs are locatedon loops at the end of the Fv regions第26页,共52页,编辑于2022年,星期五Space-filling model of(Fab)2,viewed from above,illustrating the surface location of CDR loops Light chainsGreen and brownHeavy chainsCyan and blueCDRsYellow第27页,共52页,编辑于2022年,星期五The
18、framework supports the hypervariable loopsThe framework forms a compact b barrel/sandwich with a hydrophobic coreThe hypervariable loops join,and are more flexible than,the b strandsThe sequences of the hypervariable loops are highly variable amongst antibodies of different specificitiesThe variable
19、 sequences of the hypervariable loops influences the shape,hydrophobicity and charge at the tip of the antibodyVariable amino acid sequence in the hypervariable loops accounts for the diversity of antigens that can be recognised by a repertoire of antibodiesHypervariable loops and framework:Summary第
20、28页,共52页,编辑于2022年,星期五Antigens vary in size and complexityProtein:Influenza haemagglutininHapten:5-(para-nitrophenyl phosphonate)-pentanoic acid.第29页,共52页,编辑于2022年,星期五Antibodies interact with antigens in a variety of waysAntigen inserts into a pocket in the antibodyAntigen interacts with an extended
21、antibody surface or a groove in the antibody surface第30页,共52页,编辑于2022年,星期五CH3CH2FbFvFvFvFbFvHingeElbowCH3CH2FbFvFlexibility andmotion of immunoglobulins第31页,共52页,编辑于2022年,星期五30 strongly neutralising McAb60 strongly neutralising McAb Fab regions60 weakly neutralising McAb Fab regionsHuman Rhinovirus
22、14-a common cold virus30nmModels of Human Rhinovirus 14 neutralised by monoclonal antibodies第32页,共52页,编辑于2022年,星期五Electron micrographs of Antibodies and complement opsonising Epstein Barr Virus(EBV)Negatively stained EBVEBV coated with a corona ofanti-EBV antibodiesEBV coated with antibodies and act
23、ivated complement components第33页,共52页,编辑于2022年,星期五Antibody+complement-mediated damage to E.coliHealthy E.coliElectron micrographs of the effect of antibodies and complement upon bacteria第34页,共52页,编辑于2022年,星期五Non-covalent forces inantibody-antigen interactionsElectrostatic forcesAttraction between op
24、posite chargesHydrogen bondsHydrogens shared between electronegative atomsVan der Waals forcesFluctuations in electron clouds around molecules oppositely polarise neighbouring atomsHydrophobic forcesHydrophobic groups pack together to exclude water(involves Van der Waals forces)第35页,共52页,编辑于2022年,星期
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