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Antigen processing and MHC

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Kayeen Vadakkan
Kayeen Vadakkan

Antigen processing and MHC

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Major histocompatibility Complex and antigen processing Dr.Kayeen Vadakkan
Major histocompatibility Complex • MHC molecules are membrane proteins on APCs that display peptide antigens for recognition by T lymphocytes. • In all vertebrates, the MHC contains two sets of highly polymorphic genes, called the class I and class II MHC genes. • The human MHC, called the human leukocyte antigen (HLA) complex, and the mouse MHC, called the H-2 complex. • Therefore, MHC can be classified into 3 based on structure and site of action 1. Class I MHC encode glycoproteins expressed on the surface of nearly all nucleated cells; the major function of the class I gene products is presentation of peptide antigens to TC cells 2. Class II MHC encode glycoproteins expressed primarily on antigen- presenting cells (macrophages, dendritic cells, and B cells), where they present processed antigenic peptides to TH cells 3. Class III MHC encode, in addition to other products, various secreted proteins that have immune functions, including components of the complement system and molecules involved in inflammation
Structure of MHC Molecules Class I MHC Molecules • Class I MHC molecules contain a 45-kilodalton (kDa) α chain associated noncovalently with a 12-kDa β2-microglobulin molecule. The α chain is a transmembrane glycoprotein encoded by polymorphic genes within the A, B, and C regions of the human HLA complex. β 2- Microglobulin is a protein encoded by a highly conserved gene located on a different chromosome. • The α chain is anchored in the plasma membrane by its hydrophobic transmembrane segment and hydrophilic cytoplasmic tail. • Structural analyses have revealed that the αchain of class I MHC molecules is organized into three external domains (1, 2, and 3), each containing approximately 90 amino acids; a transmembrane domain of about 25 hydrophobic amino acids followed by a short stretch of charged (hydrophilic) amino acids; and a cytoplasmic anchor segment of 30 amino acids. • The β2-microglobulin is similar in size and organization to the α3 domain; it does not contain a transmembrane region and is noncovalently bound to the class I glycoprotein. • The amino-terminal α1 and α2 domains of the α chain form two walls and a peptide-binding cleft, or groove, that can accommodate peptides typically 8 to 9 amino acids long. • The floor of the peptide-binding cleft contains amino acid residues that bind peptides for display to T lymphocytes, and the tops of the cleft walls make contact with the T cell receptor. Class II MHC Molecules • Class II MHC molecules contain two different polypeptide chains, a 33-kDa α chain and a 28- kDa β chain, which associate by noncovalent interactions • Each class II MHC molecule consists of two transmembrane chains, called α and β. Each chain has two extracellular domains, followed by the transmembrane and cytoplasmic regions. • The amino-terminal regions of both chains, called the α1 and β1 domains, contain polymorphic residues and form a cleft that is large enough to accommodate peptides of 10 to 30 residues.
Cellular Distribution of the MHC Antigens • Essentially, all nucleated cells carry classical class I molecules. • These are abundantly expressed on lymphoid cells, less so on liver, lung and kidney, and only sparsely on brain and skeletal muscle. • Class II molecules are restricted in their expression, being present only on antigen presenting cells (APCs) such as B- cells, dendritic cells and macrophages and on thymic epithelium. • When activated by agents such as interferon g, capillary endothelia and many epithelial cells in tissues other than the thymus, they can develop surface class II and increased expression of class I. Properties of MHC Genes and Proteins • MHC genes are highly polymorphic, meaning that many different alleles (variants) are present among the different individuals in the population. • MHC genes are co-dominantly expressed, meaning that the alleles inherited from both parents are expressed equally • Class I molecules are expressed on all nucleated cells, but class II molecules are expressed mainly on dendritic cells, macrophages, and B lymphocytes.
Inheritance Patterns of HLA Genes • An individual inherits one haplotype from the mother and one haplotype from the father. In outbred populations, the offspring are generally heterozygous at many loci and will express both maternal and paternal MHC alleles. • The alleles are co-dominantly expressed; that is, both maternal and paternal gene products are expressed in the same cells. • In an outbred population, each individual is generally heterozygous at each locus. • The human HLA complex is highly polymorphic and multiple alleles of each class I and class II gene exist. • When the father and mother have different haplotypes, there is a one-in-four chance that siblings will inherit the same paternal and maternal Although the rate of recombination by crossover is low within the HLA, it still contributes significantly to the diversity of the loci in human populations. • Genetic recombination generates new allelic combinations , and the high number of intervening generations since the appearance • of humans as a species has allowed extensive recombination, so that it is rare for any two unrelated individuals to have identical sets of HLA genes
Antigen Processing and Presentation • Recognition of a foreign antigen by a T cell requires that peptides derived from the antigen be displayed within the cleft of an MHC molecule on the membrane of a cell. • The formation of these peptide-MHC complexes requires that a protein antigen be degraded into peptides by a sequence of events called antigen processing. • The degraded peptides then associate with MHC molecules within the cell interior, and the peptide-MHC complexes are transported to the membrane, where they are displayed (antigen presentation). • Class I and class II MHC molecules associate with peptides that have been processed in different intracellular compartments. • Class I MHC molecules bind peptides derived from endogenous antigens that have been processed within the cytoplasm of the cell (e.g., normal cellular proteins, tumor proteins, or viral and bacterial proteins produced within infected cells). • Class II MHC molecules bind peptides derived from exogenous antigens that are internalized by phagocytosis or endocytosis and processed within the endocytic pathway. • Based on the type of cell where the processing occurs and the type of MHC the antigen processing can be classified into 1. Endogenous pathway / Cytosolic Pathway 2. Exogenous pathway / Endocytic Pathway
Endogenous pathway / Cytosolic Pathway This is the pathway by which endogenous antigens are degraded for presentation with class I MHC molecules. This occurs in four stages 1. Proteolysis of Cytosolic Proteins 2. Intake of peptides into Endoplasmic reticulum 3. Synthesis of Class I MHC and binding of peptide on it 4. Transport of Peptide-MHC Complexes to the Cell Surface
Proteolysis of Cytosolic Proteins • The peptides that bind to class I MHC molecules are derived from cytosolic proteins following digestion by the ubiquitin- proteasome pathway. • Antigenic proteins may be produced in the cytoplasm from viruses that are living inside infected cells, from some phagocytosed microbes that may leak from or be transported out of phagosomes into the cytosol, and from mutated or altered host genes that encode cytosolic or nuclear proteins, as in tumors. • These proteins are first bind to a ubiquitin molecule which unfolded the protein and take the molecule to proteosome. • This reaction, requires ATP, links several ubiquitin molecules to a lysine-amino group near the amino terminus of the protein. • Proteasome is composed of stacked rings of proteolytic enzymes that degrade the unfolded proteins into peptides.
Binding of Peptides to Class I MHC Molecules In order to form peptide-MHC complexes, the peptides must be transported into the endoplasmic reticulum (ER). The peptides produced by proteasomal digestion are in the cytosol, while the MHC molecules are being synthesized in the ER, and the two need to come together. This transport function is provided by a molecule, called the transporter associated with antigen processing (TAP), located in the ER membrane. TAP binds proteasome-generated peptides on the cytosolic side of the ER membrane, then actively pumps them into the interior of the ER. Newly synthesized class I MHC molecules, which do not contain bound peptides, associate with a bridging protein called tapasin that links them to TAP molecules in the ER membrane. Thus, as peptides enter the ER, they can easily be captured by the empty class I molecule
Synthesis of Class I MHC and peptide binding • The α chain and β 2-macroglobulin components of the class I MHC molecule are synthesized on polysomes along the rough endoplasmic reticulum. • The assembly process involves several steps and includes the participation of molecular chaperones, which facilitate the folding of polypeptides. • The first molecular chaperone involved in class I MHC assembly is calnexin, a membrane protein of the endoplasmic reticulum. • Calnexin associates with the free class I α chain and promotes its folding. • When β 2-microglobulin binds to the α chain, calnexin is released and the class I molecule associates with another chaperone calreticulin and with tapasin. • Tapasin (TAP-associated protein) brings the complex near to the TAP transporter and allows it to acquire an antigenic peptide
Transport of Peptide-MHC Complexes to the Cell Surface • Peptide loading stabilizes class I MHC molecules, which are exported to the cell surface. • Once the class I MHC molecule binds tightly to one of the peptides generated from proteasomal digestion and delivered into the ER by TAP. • This peptide-MHC complex becomes stable and is delivered to the cell surface. • If the MHC molecule does not find a peptide it can bind, the empty molecule is unstable and is eventually degraded in the ER.
Exogenous pathway / The Endocytic Pathway • This pathway is for antigens which are generated outside of cell and processed by class II MHC. This pathway can be studied in three stages 1. Internalization and Proteolysis of Antigens 2. Peptide Assembly with Class II MHC Molecules 3. Transport of Peptide-MHC Complexes to the Cell Surface
Internalization and Proteolysis of Antigens • Antigen-presenting cells can internalize antigen by phagocytosis, endocytosis, or both. • Once an antigen is internalized, it is degraded into peptides within compartments of the endocytic processing pathway. • The endocytic pathway appears to involve three increasingly acidic compartments: early endosomes (pH 6.0–6.5); late endosomes, or endolysosomes (pH 5.0–6.0); and lysosomes (pH 4.5–5.0). • Internalized antigen moves from early to late endosomes and finally to lysosomes, encountering hydrolytic enzymes and a lower pH in each compartment. • Within the compartments of the endocytic pathway, antigen is degraded into oligopeptides of about 13–18 residues, which bind to class II MHC molecules.
Peptide Assembly with Class II MHC Molecules • When class II MHC molecule are synthesized within the RER, it remains associate with a preassembled trimer of a protein called invariant chain (Ii, CD74). • This trimeric protein interacts with the peptide-binding cleft of the class II molecules, preventing any endogenously derived peptides from binding to the cleft while the class II molecule is within the RER. • Class II MHC–invariant chain complexes are transported from the RER to the endocytic pathway, moving • from early endosomes to late endosomes, and finally to lysosomes. • As the proteolytic activity increases in each successive compartment, the invariant chain is gradually degraded. However, a short fragment of the invariant chain termed CLIP (for class II–associated invariant chain peptide) remains bound to the class II molecule. • CLIP physically occupies the peptide-binding groove of the class II MHC molecule, preventing any premature binding of antigenic peptide. • The CLIP molecule will be replaced by antigen peptide catalyzed by a molecule called HLA-DM and this reaction is regulated and controlled by HLA-DO molecule.
Transport of Peptide-MHC Complexes to the Cell Surface • Peptide loading stabilizes class II MHC molecules, which are exported to the cell surface. • If a class II molecule binds a peptide with the right fit, the complex is stabilized and transported to the cell surface, where it can be recognized by a CD4+ T cell. • Class II molecules that do not find peptides they can bind are eventually degraded by lysosomal proteases

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Antigen processing and MHC

  • 1. Major histocompatibility Complex and antigen processing Dr.Kayeen Vadakkan
  • 2.
  • 3. Major histocompatibility Complex • MHC molecules are membrane proteins on APCs that display peptide antigens for recognition by T lymphocytes. • In all vertebrates, the MHC contains two sets of highly polymorphic genes, called the class I and class II MHC genes. • The human MHC, called the human leukocyte antigen (HLA) complex, and the mouse MHC, called the H-2 complex. • Therefore, MHC can be classified into 3 based on structure and site of action 1. Class I MHC encode glycoproteins expressed on the surface of nearly all nucleated cells; the major function of the class I gene products is presentation of peptide antigens to TC cells 2. Class II MHC encode glycoproteins expressed primarily on antigen- presenting cells (macrophages, dendritic cells, and B cells), where they present processed antigenic peptides to TH cells 3. Class III MHC encode, in addition to other products, various secreted proteins that have immune functions, including components of the complement system and molecules involved in inflammation
  • 4. Structure of MHC Molecules Class I MHC Molecules • Class I MHC molecules contain a 45-kilodalton (kDa) α chain associated noncovalently with a 12-kDa β2-microglobulin molecule. The α chain is a transmembrane glycoprotein encoded by polymorphic genes within the A, B, and C regions of the human HLA complex. β 2- Microglobulin is a protein encoded by a highly conserved gene located on a different chromosome. • The α chain is anchored in the plasma membrane by its hydrophobic transmembrane segment and hydrophilic cytoplasmic tail. • Structural analyses have revealed that the αchain of class I MHC molecules is organized into three external domains (1, 2, and 3), each containing approximately 90 amino acids; a transmembrane domain of about 25 hydrophobic amino acids followed by a short stretch of charged (hydrophilic) amino acids; and a cytoplasmic anchor segment of 30 amino acids. • The β2-microglobulin is similar in size and organization to the α3 domain; it does not contain a transmembrane region and is noncovalently bound to the class I glycoprotein. • The amino-terminal α1 and α2 domains of the α chain form two walls and a peptide-binding cleft, or groove, that can accommodate peptides typically 8 to 9 amino acids long. • The floor of the peptide-binding cleft contains amino acid residues that bind peptides for display to T lymphocytes, and the tops of the cleft walls make contact with the T cell receptor. Class II MHC Molecules • Class II MHC molecules contain two different polypeptide chains, a 33-kDa α chain and a 28- kDa β chain, which associate by noncovalent interactions • Each class II MHC molecule consists of two transmembrane chains, called α and β. Each chain has two extracellular domains, followed by the transmembrane and cytoplasmic regions. • The amino-terminal regions of both chains, called the α1 and β1 domains, contain polymorphic residues and form a cleft that is large enough to accommodate peptides of 10 to 30 residues.
  • 5. Cellular Distribution of the MHC Antigens • Essentially, all nucleated cells carry classical class I molecules. • These are abundantly expressed on lymphoid cells, less so on liver, lung and kidney, and only sparsely on brain and skeletal muscle. • Class II molecules are restricted in their expression, being present only on antigen presenting cells (APCs) such as B- cells, dendritic cells and macrophages and on thymic epithelium. • When activated by agents such as interferon g, capillary endothelia and many epithelial cells in tissues other than the thymus, they can develop surface class II and increased expression of class I. Properties of MHC Genes and Proteins • MHC genes are highly polymorphic, meaning that many different alleles (variants) are present among the different individuals in the population. • MHC genes are co-dominantly expressed, meaning that the alleles inherited from both parents are expressed equally • Class I molecules are expressed on all nucleated cells, but class II molecules are expressed mainly on dendritic cells, macrophages, and B lymphocytes.
  • 6. Inheritance Patterns of HLA Genes • An individual inherits one haplotype from the mother and one haplotype from the father. In outbred populations, the offspring are generally heterozygous at many loci and will express both maternal and paternal MHC alleles. • The alleles are co-dominantly expressed; that is, both maternal and paternal gene products are expressed in the same cells. • In an outbred population, each individual is generally heterozygous at each locus. • The human HLA complex is highly polymorphic and multiple alleles of each class I and class II gene exist. • When the father and mother have different haplotypes, there is a one-in-four chance that siblings will inherit the same paternal and maternal Although the rate of recombination by crossover is low within the HLA, it still contributes significantly to the diversity of the loci in human populations. • Genetic recombination generates new allelic combinations , and the high number of intervening generations since the appearance • of humans as a species has allowed extensive recombination, so that it is rare for any two unrelated individuals to have identical sets of HLA genes
  • 7. Antigen Processing and Presentation • Recognition of a foreign antigen by a T cell requires that peptides derived from the antigen be displayed within the cleft of an MHC molecule on the membrane of a cell. • The formation of these peptide-MHC complexes requires that a protein antigen be degraded into peptides by a sequence of events called antigen processing. • The degraded peptides then associate with MHC molecules within the cell interior, and the peptide-MHC complexes are transported to the membrane, where they are displayed (antigen presentation). • Class I and class II MHC molecules associate with peptides that have been processed in different intracellular compartments. • Class I MHC molecules bind peptides derived from endogenous antigens that have been processed within the cytoplasm of the cell (e.g., normal cellular proteins, tumor proteins, or viral and bacterial proteins produced within infected cells). • Class II MHC molecules bind peptides derived from exogenous antigens that are internalized by phagocytosis or endocytosis and processed within the endocytic pathway. • Based on the type of cell where the processing occurs and the type of MHC the antigen processing can be classified into 1. Endogenous pathway / Cytosolic Pathway 2. Exogenous pathway / Endocytic Pathway
  • 8. Endogenous pathway / Cytosolic Pathway This is the pathway by which endogenous antigens are degraded for presentation with class I MHC molecules. This occurs in four stages 1. Proteolysis of Cytosolic Proteins 2. Intake of peptides into Endoplasmic reticulum 3. Synthesis of Class I MHC and binding of peptide on it 4. Transport of Peptide-MHC Complexes to the Cell Surface
  • 9. Proteolysis of Cytosolic Proteins • The peptides that bind to class I MHC molecules are derived from cytosolic proteins following digestion by the ubiquitin- proteasome pathway. • Antigenic proteins may be produced in the cytoplasm from viruses that are living inside infected cells, from some phagocytosed microbes that may leak from or be transported out of phagosomes into the cytosol, and from mutated or altered host genes that encode cytosolic or nuclear proteins, as in tumors. • These proteins are first bind to a ubiquitin molecule which unfolded the protein and take the molecule to proteosome. • This reaction, requires ATP, links several ubiquitin molecules to a lysine-amino group near the amino terminus of the protein. • Proteasome is composed of stacked rings of proteolytic enzymes that degrade the unfolded proteins into peptides.
  • 10. Binding of Peptides to Class I MHC Molecules In order to form peptide-MHC complexes, the peptides must be transported into the endoplasmic reticulum (ER). The peptides produced by proteasomal digestion are in the cytosol, while the MHC molecules are being synthesized in the ER, and the two need to come together. This transport function is provided by a molecule, called the transporter associated with antigen processing (TAP), located in the ER membrane. TAP binds proteasome-generated peptides on the cytosolic side of the ER membrane, then actively pumps them into the interior of the ER. Newly synthesized class I MHC molecules, which do not contain bound peptides, associate with a bridging protein called tapasin that links them to TAP molecules in the ER membrane. Thus, as peptides enter the ER, they can easily be captured by the empty class I molecule
  • 11. Synthesis of Class I MHC and peptide binding • The α chain and β 2-macroglobulin components of the class I MHC molecule are synthesized on polysomes along the rough endoplasmic reticulum. • The assembly process involves several steps and includes the participation of molecular chaperones, which facilitate the folding of polypeptides. • The first molecular chaperone involved in class I MHC assembly is calnexin, a membrane protein of the endoplasmic reticulum. • Calnexin associates with the free class I α chain and promotes its folding. • When β 2-microglobulin binds to the α chain, calnexin is released and the class I molecule associates with another chaperone calreticulin and with tapasin. • Tapasin (TAP-associated protein) brings the complex near to the TAP transporter and allows it to acquire an antigenic peptide
  • 12. Transport of Peptide-MHC Complexes to the Cell Surface • Peptide loading stabilizes class I MHC molecules, which are exported to the cell surface. • Once the class I MHC molecule binds tightly to one of the peptides generated from proteasomal digestion and delivered into the ER by TAP. • This peptide-MHC complex becomes stable and is delivered to the cell surface. • If the MHC molecule does not find a peptide it can bind, the empty molecule is unstable and is eventually degraded in the ER.
  • 13. Exogenous pathway / The Endocytic Pathway • This pathway is for antigens which are generated outside of cell and processed by class II MHC. This pathway can be studied in three stages 1. Internalization and Proteolysis of Antigens 2. Peptide Assembly with Class II MHC Molecules 3. Transport of Peptide-MHC Complexes to the Cell Surface
  • 14. Internalization and Proteolysis of Antigens • Antigen-presenting cells can internalize antigen by phagocytosis, endocytosis, or both. • Once an antigen is internalized, it is degraded into peptides within compartments of the endocytic processing pathway. • The endocytic pathway appears to involve three increasingly acidic compartments: early endosomes (pH 6.0–6.5); late endosomes, or endolysosomes (pH 5.0–6.0); and lysosomes (pH 4.5–5.0). • Internalized antigen moves from early to late endosomes and finally to lysosomes, encountering hydrolytic enzymes and a lower pH in each compartment. • Within the compartments of the endocytic pathway, antigen is degraded into oligopeptides of about 13–18 residues, which bind to class II MHC molecules.
  • 15. Peptide Assembly with Class II MHC Molecules • When class II MHC molecule are synthesized within the RER, it remains associate with a preassembled trimer of a protein called invariant chain (Ii, CD74). • This trimeric protein interacts with the peptide-binding cleft of the class II molecules, preventing any endogenously derived peptides from binding to the cleft while the class II molecule is within the RER. • Class II MHC–invariant chain complexes are transported from the RER to the endocytic pathway, moving • from early endosomes to late endosomes, and finally to lysosomes. • As the proteolytic activity increases in each successive compartment, the invariant chain is gradually degraded. However, a short fragment of the invariant chain termed CLIP (for class II–associated invariant chain peptide) remains bound to the class II molecule. • CLIP physically occupies the peptide-binding groove of the class II MHC molecule, preventing any premature binding of antigenic peptide. • The CLIP molecule will be replaced by antigen peptide catalyzed by a molecule called HLA-DM and this reaction is regulated and controlled by HLA-DO molecule.
  • 16. Transport of Peptide-MHC Complexes to the Cell Surface • Peptide loading stabilizes class II MHC molecules, which are exported to the cell surface. • If a class II molecule binds a peptide with the right fit, the complex is stabilized and transported to the cell surface, where it can be recognized by a CD4+ T cell. • Class II molecules that do not find peptides they can bind are eventually degraded by lysosomal proteases