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Antibody ( immunoglobulin) Serum protein electrophoresis (SEP) Serum protein electrophoresis (SEP) Basic structure and function of immunoglobulin. Basic structure and function of immunoglobulin. Monoclonal antibody, its modification and application Monoclonal antibody, its modification and application
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Serum protein electrophoresis (SEP)
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Buffer pH 8.6
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Serum electrophoresis
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Immunoglobulin (antibody, BCR): universal adaptor
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典型抗體分子的構造 (1) BCR and Ab BCR and Ab 構造功能 異 C 端序 列 作用 機制 同 免疫球 蛋白 辨識 抗原 C 端 N 端
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Proteolytic digestion of IgG Variable region Fab: papain digest F(ab')2: pepsin digest Constant region (Fc)
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Different domains have different functions
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抗體分子與專一性抗原之交 互作用 (1) 局部區域的高度 變異序列形成抗 原結合位 局部區域的高度 變異序列形成抗 原結合位 Hypervariable region Framework region CDR (complementarity- determining region)
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General structures of five classes of antibody
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Structure and formation of secretory IgA
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Antigenic determinants of immunoglobulin Isotypes: all variants present in serum of normal individual types: heavy and light chain classes: IgG, IgA, IgM, IgD, IgE subclasses: IgG1, IgG2, IgG3, IgG4 subgroups: VHI, VHII, VHIII Allotypes : genetically controlled alternative forms Idiotypes : individually specific to each immunoglobulin molecule
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Immunoglobulin superfamily
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Generation of diversity (G.O.D.) VDJ rearrangement of heavy chain VDJ rearrangement of heavy chain VJ rearrangement of light chain VJ rearrangement of light chain random combination of heavy and light chain random combination of heavy and light chain Imprecision of rearrangement Imprecision of rearrangement
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V-region genes are constructed from gene segments
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Overview of B cell development
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Model of allelic exclusion
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Immunoglobulin concentration changes along the age
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Serum immunoglobulin vary among different healthy persons IgG: 800-1600 mg/dl IgA: 140-400 mg/dl IgM: 50-200mg/dl IgD: 0-40 mg/dl
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Antibody response Clonal selection Clonal selection Primary and secondary antibody response Primary and secondary antibody response Isotype switch: IgM----->IgG Affinity maturation: Somatic mutation
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Monoclonal antibody Myeloma (HGPRT-) Spleen from immunized mice HAT medium Selection Limiting dilution and cloning
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Method Immunization with antigen Spleen and myeloma cell fusion Polyethylene glycol (PEG): polymer of ethylene oxide HAT medium: selection of hybridoma Screening Cloning by limiting dilution: Poisson distribution Large scale production and storage: can be purified by protein A affinity column cell line (10-50 g/ml) ascites (1-10 mg/ml)
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NUCLEOTIDES DNA RNA HGPRT Hypoxanthine TK Thymidine Secondary Pathway Normal splenocyle spontaneous death ACTIVE GROWTH Enzyme-deficient (HGPRT-) myeloma cell HAT-dependent death ~~~~~~~~~~~~~~~~~~~~~~ Main pathway (de novo) Aminopterin Block Hybrid cell
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Application of monoclonal antibodies: universal adaptor Antigen purification: affinity column Antigen purification: affinity column Diagnosis: detect Ag or Ab Diagnosis: detect Ag or Ab pathogen pathogen cell surface marker cell surface marker soluble antigens e.g. AFP soluble antigens e.g. AFP cancer diagnosis: immunoimaging cancer diagnosis: immunoimaging Immunotherapy Immunotherapy Cancer therapy Cancer therapy Autoimmune disease treatment Autoimmune disease treatment Allergy prevention Allergy prevention Tissue transplantation Tissue transplantation
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Application of monoclonal antibody
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Application of mAb as immunotherapeutic drugs
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Monoclonal antibodies that recognize tumor- specific antigens might be used in a variety of ways to help eliminate tumors
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MAT: the magic bullet Therapeutic results were disappointing until recently. Therapeutic results were disappointing until recently. Two major hurdles were encountered. Two major hurdles were encountered. Biologic activity in humans severely limited due to the host ’ s immune response to foreign mAbs (production of human anti-mouse Abs). Causes neutralization of activity and toxicity. Biologic activity in humans severely limited due to the host ’ s immune response to foreign mAbs (production of human anti-mouse Abs). Causes neutralization of activity and toxicity. Large-scale production Large-scale production
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Mouse mAb may cause serum sickness in vivo
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Approaches to reduce or eliminate human anti-mouse antibodies. Chimeric Antibodies Chimeric Antibodies Cloned antibody genes are generated in which the variable regions from the original mouse mAb are combined with human antibody- constant regions. Cloned antibody genes are generated in which the variable regions from the original mouse mAb are combined with human antibody- constant regions. Highly effective in reducing human anti- mouse antibodies (HAMA). However, the variable (Ag-recognition) domains are still foreign; HAMA often still occurs neutralizing efficacy. Highly effective in reducing human anti- mouse antibodies (HAMA). However, the variable (Ag-recognition) domains are still foreign; HAMA often still occurs neutralizing efficacy.
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Generation of chimeric mouse-human mAb
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Antibodies can be engineered to reduce their immunogenicity in humans Red: mouseWhite: human chimaetic humanized
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Chimeric Antibodies
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Humanized mAbs All portions of the mAb not required for antigen binding, including framework residues in the variable region, are replaced with human sequences. All portions of the mAb not required for antigen binding, including framework residues in the variable region, are replaced with human sequences. Gene engineering, expression, evaluation Gene engineering, expression, evaluation < 10% of optimized mAb retains mouse sequence < 10% of optimized mAb retains mouse sequence Highly-effective (but time-consuming) approach Highly-effective (but time-consuming) approach
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抗體分子與專一性抗原之交 互作用 局部區域的高度 變異序列形成抗 原結合位 局部區域的高度 變異序列形成抗 原結合位 Hypervariable region Framework region CDR (complementarity- determining region)
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Humanized mAb CDR: complementary determination region
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Antibodies can be engineered to reduce their immunogenicity in humans Red: mouseWhite: human chimaetic humanized
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Modification of mouse mAb
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Antibodies in action
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MAT in Organ Transplantation Rejection of allografts is an immunological response exerted primarily by T-cells. mAb approaches against T-cell antigens has proven effective. Rejection of allografts is an immunological response exerted primarily by T-cells. mAb approaches against T-cell antigens has proven effective. CD25 (IL2-Receptor chain). Highly effective approach for the prevention of graft rejection episodes and graft loss (e.g., renal). CD25 (IL2-Receptor chain). Highly effective approach for the prevention of graft rejection episodes and graft loss (e.g., renal). basiliximab (chimeric) basiliximab (chimeric) dacliximab (humanized) dacliximab (humanized)
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MAT in Coronary Artery Disease Atherosclerotic lesions (plaques) involve platelet aggregation followed by coagulation and thrombus formation. Platelet receptors involved in early steps of plaque formation. Atherosclerotic lesions (plaques) involve platelet aggregation followed by coagulation and thrombus formation. Platelet receptors involved in early steps of plaque formation. basis of “ one-aspirin-a-day ” concept basis of “ one-aspirin-a-day ” concept limited efficacy in preventing platelet aggregation limited efficacy in preventing platelet aggregation Abciximab (chimeric mAb) has been developed/approved as an effective treatment for the prevention of thrombosis and plaque formation in high risk patients. Abciximab (chimeric mAb) has been developed/approved as an effective treatment for the prevention of thrombosis and plaque formation in high risk patients. Targets the platelet receptors (integrins) Targets the platelet receptors (integrins) Prevents platelet aggregation Prevents platelet aggregation
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MAT in Autoimmune Diseases TNF is a proinflammatory cytokine that has been implicated as a causal factor in a variety of inflammatory diseases including Rheumatoid Arthritis. TNF is a proinflammatory cytokine that has been implicated as a causal factor in a variety of inflammatory diseases including Rheumatoid Arthritis. Infliximab is a chimeric mAb targeted to TNF . has displayed remarkable activity against Rheumatoid Arthritis and other inflammatory diseases (Crohn ’ s Disease). Infliximab is a chimeric mAb targeted to TNF . has displayed remarkable activity against Rheumatoid Arthritis and other inflammatory diseases (Crohn ’ s Disease). Approved in 1998. First for Crohn ’ s Disease; now R.A. Approved in 1998. First for Crohn ’ s Disease; now R.A.
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Antibodies can be used to alleviate and suppress autoimmune disease Anti-inflammatory effects of anti-TNF- therapy in rheumatoid arthritis
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MAT in Cancer (I) Most intensively studied area (25 years of research). Most intensively studied area (25 years of research). Cancer poses the highest hurdles. Cancer poses the highest hurdles. Also being evaluated in modified versions involving the conjugation to radio-ionizing particles, immunotoxins, immunoliposomes. Also being evaluated in modified versions involving the conjugation to radio-ionizing particles, immunotoxins, immunoliposomes.
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MAT in Cancer (II) Rituximab (chimeric mAb) Rituximab (chimeric mAb) Targets CD20; a cell surface protein expressed exclusively on B cells. Targets CD20; a cell surface protein expressed exclusively on B cells. Approved for the treatment of B cell malignancies (NHL, CLL, ALL). Approved for the treatment of B cell malignancies (NHL, CLL, ALL). Trastuzumab (humanized mAb) Trastuzumab (humanized mAb) Her2 is a form of the EGF-Receptor that undergoes amplification in approximately 25% of breast cancers. Her2 is a form of the EGF-Receptor that undergoes amplification in approximately 25% of breast cancers. 1st identified as a rat oncogene called neu (HER2/neu) 1st identified as a rat oncogene called neu (HER2/neu) Patients with amplified HER2 expression suffer a very poor prognosis. Patients with amplified HER2 expression suffer a very poor prognosis. Trastuzumab (Herceptin) has displayed impressive activity against HER2+ breast cancer both alone and in combination. Trastuzumab (Herceptin) has displayed impressive activity against HER2+ breast cancer both alone and in combination.
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Summary Antibodies are universal adaptors which can bind to any specific target both in vitro and in vivo. Antibodies are universal adaptors which can bind to any specific target both in vitro and in vivo. Humanized monoclonal antibody reduce its immunogenecity without change its specificity. Humanized monoclonal antibody reduce its immunogenecity without change its specificity. MAT provides another way to develop new therapy against cancer, autoimmune disease … etc. (serum therapy) MAT provides another way to develop new therapy against cancer, autoimmune disease … etc. (serum therapy)
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New approaches under development Phage-display libraries expressing human VH and VL chains are assembled into libraries and expressed as combinatorial matrices. Phage-display libraries expressing human VH and VL chains are assembled into libraries and expressed as combinatorial matrices. Assayed for immunoreactivity against antigen of interest. Assayed for immunoreactivity against antigen of interest. Transgenic Mouse Approach Transgenic Mouse Approach A procedure in which the endogenous mouse Ig gene loci is replaced by homologous recombination with their human homologs. A procedure in which the endogenous mouse Ig gene loci is replaced by homologous recombination with their human homologs. Immunization of transgenic mouse followed by standard hybridoma procedures produces a fully humanized mAb. Immunization of transgenic mouse followed by standard hybridoma procedures produces a fully humanized mAb.
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Advantages of phage display More efficiently than through conventional hybridoma system. More efficiently than through conventional hybridoma system. Cheaper to produce recombinant antibodies using bacteria, rather than mammalian cell line. Cheaper to produce recombinant antibodies using bacteria, rather than mammalian cell line. Easier to maintain and grow bacterial cultures for recombinant antibody production. Easier to maintain and grow bacterial cultures for recombinant antibody production. Bypass immunization in antibody selection. Bypass immunization in antibody selection. Bypass the use of animal cells for production of antibodies. Bypass the use of animal cells for production of antibodies. Producing the combinatorial library (ideally with 10 8 to 10 9 members) of functional antibodies to generate a larger repertoire of antibodies than those available through conventional hybridoma technology. Producing the combinatorial library (ideally with 10 8 to 10 9 members) of functional antibodies to generate a larger repertoire of antibodies than those available through conventional hybridoma technology. Easy isolation and expression of the cloned gene in a bacterial host. Easy isolation and expression of the cloned gene in a bacterial host. Excellent potential to further improve binding properties of the selected antibody by protein engineering techniques. Excellent potential to further improve binding properties of the selected antibody by protein engineering techniques.
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PNAS 101:2536, 2004 Feb.
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Selection of phage library and screening of phage antibodies Two human nonimmune single-chain variable region fragment (scFv) libraries (a total of 2.7x10 10 members) constructed from B cells of 57 unimmunized donors were used for selection of scFvs against the purified S1-C9
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Generation human mAb by transgenic mice
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