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IMMUNOGENETICS
Mohamed Labib Salem
Prof. of Immunology
Faculty of Science, Tanta University
Talk Agenda
1. Definition of immunogenetics
2. Basic of immune responses
o Innate immunity
o Adaptive immunity
3. Diversity for specificity
o BCR
o TCR
o HLA
4. Diseases associated with
immunodeficiency
How are re we different and why?
How are re we different and why?
Talk Agenda
1. Definition of immunogenetics
2. Basic of immune responses
o Innate immunity
o Adaptive immunity
3. Diversity for specificity
o BCR
o TCR
o HLA
4. Diseases associated with
immunodeficiency
Immunogenetics as a discipline
The study of the genetic control
of the cells and molecules that
shapes immune responses
against infectious
microorganisms
Immunogenetics as a discipline
It focuses on:
1. Structure and organizations of genes
mediating immune responses
2. HLA antigens and their association
with disease
3. Generation of antibody diversity
4. Generation of T cell diversity
Immunogenetics: Specificity
1. Specificity: Is a key feature of the
adaptive immune system
2. Ability of the immune system to
distinguish between antigens
3. It ensures that distinct antigens
elicit specific responses
Polymorphism
• The human genome contains an estimated 32,000 genes
that encode mRNAs for proteins.
• To protect us, our immune system has the ability to
produce about 1010-1011 different antibodies.
• How can our immune system produce so many different
antibodies with so few genes?
• How is Ig diversity specified genetically?
Polymorphism→ diversity
Immunogenetics
• Specificity and polymorphism
– specificity is attributed to highly variable
lymphocyte receptors ( BCR and TCR ) and
immunoglobulins
– Unique specificity of antigen receptors and the
ability to react selectively against a very broad
range of foreign antigens is a result of
polymorphism
– Polymorphism means existence of two or more
alternative forms or variants of expressed proteins
in a population
Talk Agenda
1. Definition of immunogenetics
2. Basic of immune responses
o Innate immunity
o Adaptive immunity
3. Diversity for specificity
o BCR
o TCR
o HLA
4. Diseases associated with
immunodeficiency
Because of too many
antigen we need to too
many specificities
“Diversity”
Antigens
Antigen
Recognition • Antigens
 Processed, Unprocessed
 Endogenous, exogenous
 Self, Foreign
• Receptors
 Ag-specific adaptive
 PRRs ->innate
Innate
&
Adaptive
Immune
Cells
Levels of immune response
Talk Agenda
1. Definition of immunogenetics
2. Basic of immune responses
o Innate immunity
o Adaptive immunity
3. Diversity for specificity
o BCR
o TCR
o HLA
4. Diseases associated with
immunodeficiency
MHC restriction of immune response
TCR/BCR TCR/BCR
Immunogenetics
• Immunoglobulin superfamily
Polymorphic immune molecules belong
to a large family of proteins that contain a
globular structure motif - Ig domain.
they all possess a domain known as an
immunoglobulin domain or fold
This group of proteins is called
immunoglobulin super family
• There are about 40 members of immunoglobulin
superfamily:
– Recognition and regulation molecules:
• Ig, BCR, TCR, MHC molecules, CD2, CD3, CD4, CD8
molécules, Fc receptors
– Adhesion molecules (e.g. ICAM-1, ICAM-2,
VCAM-1, PECAM-1)
– Receptors for PDGFR (= platelet growth factor
receptor)
– Transporter associated with antigens (TAPI and TAO2)
Immunogenetics
• Immunoglobulin gene superfamily
– Genes that encode immunoglobulins (antibodies) ;
BCR, TCR on cell surface molecules ; and MHC
molecules
– Appear to be evolutionary related genes
– Members of a family share a certain degree of
sequence homology
– Are likely to have been derived from a common
precursor gene
Immunogenetics
• The most polymorphic molecules of the human immune
system
Immunoglobulins
[antibodies]
MHC molecules
[membrane
glycoproteins]
TCR
(T-Cell Receptor)
BCR
(B-Cell Receptor)
Members of the
immunoglobulin
superfamily
Immunogenetics
GENES encoding Ig, BCR and TCR: germline
organization
Cell and Xsome carrying the genes
Ig (BCR) Heavy chain locus B-cell, Chromosome # 14
Ig (BCR) Light chain locus B-cell, Xsome # 2 (k), 22 (l)
TCR b chain T-cell, Xsome # 7
TCR a chain T-cell, Xsome # 14
MHC class I genes All nucleated Xsome # 6
MHC class II genes APC, Xsome # 6
BCR, TCR
BCR, TCR
Antibody Molecules
• The molecule has a "Y" shape,
with the two ends of the fork
• 2 heavy chains plus 2 light
chains, joined together by
disulfide bridges.
• Variable (V) regions form antigen
binding sites which specifically
bind particular antigens
• Each Ab molecule has 2 identical
Ag binding regions, and thus the
Ab molecules can bind together
large groups of Ag's.
• Each light (L) chain has 2 domains, a variable (V) region and
a constant (C) region.
– There are only a small number of C regions in each
person, but there are very many different V regions.
– Note that the V and C regions are together on the same
polypeptide chain!
• Each heavy (H) chain has 4 domains, a V domain followed
by 3 C domains.
• The C domains determine the 5 classes of antibodies: IgM
(early response), IgG (main blood Ig), IgA (in body
secretions), IgE (allergic response), and IgD (mostly a cell
surface molecule in the early response).
• In many cases, the constant class-specific regions of the H
chains bind to receptors on the surface of specific cells.
For instance, IgA binds to secretory cells so it gets secreted
into tears, mucus, etc.
Antibody Molecules
• Genes for immunoglobulin (antibodies)
– Expression of genes for Ig occurs in B-cells
– Antibody genes are composed of segments
– Gene of Ig heavy chain …chromosome 14
– Genes for Ig kappa and lambda on chromosome 2
and 22 respectively
Antibody Molecules
BCR genetics
D-diversity, J-joining, V-variability, C-constant
Chromosome 14
– During B-cell maturation in the bone marrow, Ig gene
segments are rearranged and generated into more
than 1010 combinations of V region.
– Each B cell has a unique combination and is
antigenically committed to a specific epitope.
– After antigenic stimulation, further rearrangement of
C-region gene segments can generate changes in
isotypes without changing the specificity of Ig.
– Genomic rearrangement is an essential feature of
lymphocyte differentiation, and no other vertebrate
cell type has been shown to undergo this process.
Antibody Molecules
Generation of diversity
• Antigens – 1011 (100 billion)
• Mechanisms – before and after contact with antigen
 V(D)J recombination
 Junctional diversity
 Combinations of receptor chains
 Somatic hypermutation (affinity maturation)
TCR genetics
chain chromosome V D J C
α 14 50 - 70 1
β 7 57 2 13 2
Major Histocompatibility Complex
(MHC)
• The MHC is a closely linked complex of genes that govern
production of histocompatibility between individuals and
species.
• In humans, MHC resides on the short arm of
chromosome 6
• Class I MHC (HLA) proteins are coded in 3 genes (HLA-A,
HLA-B, HLA-C)
• Class II MHC (HLA-D) proteins are code in several loci
(DP, DQ and DR)
• HLA genes are very diverse (polymorphic) i.e. there are
many alleles of the class I and II genes
MHC Molecules
• Between the class I and class II gene loci,
there is a third locus (Class III)
• This locus contains genes encoding tumor
necrosis factor, lymphotoxin and two
complement components (C2 and C4)
• Class III antigens do not participate in MHC
restriction or graft rejection
Gene structure
Location and components
Class I MHC
Class II MHC
RBCs
Professional
APCs
Nucleated cells
A, B, C DP, DQ, DR
Class III codes for other proteins eg complement components, cytokines
Class I MHC
• α chain (43kDa), β2 microglobulin (12 kDa)
• β2-microglobulin – genes on chromosome 15
• Can accommodate 10 amino acids
b2-M
a-chain
Peptide
Class II MHC
a-chain
b-chain
Peptide
• α chain (34kDa), β chain (29 kDa)
• Can accommodate ~15 amino acids
Class I MHC and Class II MHC
MHC Class I MHC Class II
Nomenclature HLA-A, HLA-B, HLA-C HLA-DP, HLA-DQ,
HLA-DR
Found on All nucleated somatic cells Macrophages, B-cells,
Dentritic cells, langerhans
cells of skin and activated
T cells
Recognized by CD8 TC cells CD4 TH cells
Functions Presentation of Ag to TC
cells leading to elimination
of tumor or infected host
cell
Presentation of Ag to TH
cells which secrete
cytokines
Polymorphism
Application of HLA in medicine
Transplantation
Forensic medicine
Anthropological studies
Regulating immune responses
Disease association
Talk Agenda
1. Definition of immunogenetics
2. Basic of immune responses
o Innate immunity
o Adaptive immunity
3. Diversity for specificity
o BCR
o TCR
o HLA
4. Diseases associated with
immunodeficiency
impaired function of the immune system (immunodeficiency) resulting in increased
susceptibility to infection.
IMMUNODEFICIENCY
Primary immunodeficiency-PID
intrinsic defect of a component of the immune Most by defects in single genes and are hence
heritable.. rare
Secondary or acquired
secondary to another pathological condition, which adversely affects immune function,
CAUSES
1. DNA DAMAGE
From a clinical perspective, immuno- deficiencies can be classified into eight categories
T AND B CELL IMMUNODEFICIENCIES
Next slide
SCID; CLASSIFICATION
About 15 percent of SCID cases are caused by deficiency of adenosine deaminase (ADA), an enzyme
required for the salvage of nucleotides within lymphoid cells. The lack of ADA causes the accumulation of
toxic metabolites of adenosine (deoxy- adenosine and deoxy-ATP) within lymphoid cells, resulting in their
demise.
NO STEM CELLS
Mutations of the tyro-sine phosphatase,
CD45, which helps to initiate signaling by the
TCR, results in T−B+ SCID in humans. Mutation
of components of CD3-complex (CD3 γ, ε, and
δ) result in a SCID phenotype. During signal
transduction via TCRs, the protein tyrosine
kinases Lck and ZAP70 are required for
phosphorylation of ITAMs on the intracy-
toplasmic segment of the TCR. Deficiency of
either of these kinases results in rare forms of
SCID.
T AND B CELL IMMUNODEFICIENCIES
Defects in Leucocyte Migration
protein lymphocyte function-associated antigen-1(LFA-1) LFA- 1 expressed on the
leucocyte surface and its ligand intercellular adhesion molecule- 1 (ICAM-1)
expressed on the luminal surface of activated endothelial cells.
•a common β chain (CD18) with three separate α chains called CD11a, b, and c.
•CD18-CD11a heterodimers form LFA-1,
LAD1 n LAD2
 CD18/CD11b Heterodimers form complement receptor 3, (CR3)
 CD18 combined to CD11c forms complement receptor 4 (CR4).
Mutation of the gene encoding CD18 (resulting in the lack of expression of LFA-1,
CR3, and CR4) results in an inherited primary immunodeficiency called leukocyte
adhesion deficiency type 1(LAD1).
sialyl LewisX, which is expressed on the surface of leucocytes,
LAD1
LAD2
ANTIBODY DEFICIENCY DISEASES
Brutons tyrosine kinase
Ab switch, memory b cells, somatic hypermutation, dendritic cells to prime t
cells,CD80 n 86 upregulation
HYPER IgM SYNDROMES
Disease association
6-Feb-21 PEH 210 67

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Immunogenetics by Prof. Mohamed Labib Salem Tanta University

  • 1. IMMUNOGENETICS Mohamed Labib Salem Prof. of Immunology Faculty of Science, Tanta University
  • 2. Talk Agenda 1. Definition of immunogenetics 2. Basic of immune responses o Innate immunity o Adaptive immunity 3. Diversity for specificity o BCR o TCR o HLA 4. Diseases associated with immunodeficiency
  • 3. How are re we different and why?
  • 4. How are re we different and why?
  • 5. Talk Agenda 1. Definition of immunogenetics 2. Basic of immune responses o Innate immunity o Adaptive immunity 3. Diversity for specificity o BCR o TCR o HLA 4. Diseases associated with immunodeficiency
  • 6. Immunogenetics as a discipline The study of the genetic control of the cells and molecules that shapes immune responses against infectious microorganisms
  • 7. Immunogenetics as a discipline It focuses on: 1. Structure and organizations of genes mediating immune responses 2. HLA antigens and their association with disease 3. Generation of antibody diversity 4. Generation of T cell diversity
  • 8. Immunogenetics: Specificity 1. Specificity: Is a key feature of the adaptive immune system 2. Ability of the immune system to distinguish between antigens 3. It ensures that distinct antigens elicit specific responses
  • 9. Polymorphism • The human genome contains an estimated 32,000 genes that encode mRNAs for proteins. • To protect us, our immune system has the ability to produce about 1010-1011 different antibodies. • How can our immune system produce so many different antibodies with so few genes? • How is Ig diversity specified genetically? Polymorphism→ diversity
  • 10. Immunogenetics • Specificity and polymorphism – specificity is attributed to highly variable lymphocyte receptors ( BCR and TCR ) and immunoglobulins – Unique specificity of antigen receptors and the ability to react selectively against a very broad range of foreign antigens is a result of polymorphism – Polymorphism means existence of two or more alternative forms or variants of expressed proteins in a population
  • 11. Talk Agenda 1. Definition of immunogenetics 2. Basic of immune responses o Innate immunity o Adaptive immunity 3. Diversity for specificity o BCR o TCR o HLA 4. Diseases associated with immunodeficiency
  • 12. Because of too many antigen we need to too many specificities “Diversity”
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  • 19. Antigen Recognition • Antigens  Processed, Unprocessed  Endogenous, exogenous  Self, Foreign • Receptors  Ag-specific adaptive  PRRs ->innate
  • 21. Levels of immune response
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  • 23. Talk Agenda 1. Definition of immunogenetics 2. Basic of immune responses o Innate immunity o Adaptive immunity 3. Diversity for specificity o BCR o TCR o HLA 4. Diseases associated with immunodeficiency
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  • 25. MHC restriction of immune response TCR/BCR TCR/BCR
  • 26. Immunogenetics • Immunoglobulin superfamily Polymorphic immune molecules belong to a large family of proteins that contain a globular structure motif - Ig domain. they all possess a domain known as an immunoglobulin domain or fold This group of proteins is called immunoglobulin super family
  • 27. • There are about 40 members of immunoglobulin superfamily: – Recognition and regulation molecules: • Ig, BCR, TCR, MHC molecules, CD2, CD3, CD4, CD8 molécules, Fc receptors – Adhesion molecules (e.g. ICAM-1, ICAM-2, VCAM-1, PECAM-1) – Receptors for PDGFR (= platelet growth factor receptor) – Transporter associated with antigens (TAPI and TAO2) Immunogenetics
  • 28. • Immunoglobulin gene superfamily – Genes that encode immunoglobulins (antibodies) ; BCR, TCR on cell surface molecules ; and MHC molecules – Appear to be evolutionary related genes – Members of a family share a certain degree of sequence homology – Are likely to have been derived from a common precursor gene Immunogenetics
  • 29. • The most polymorphic molecules of the human immune system Immunoglobulins [antibodies] MHC molecules [membrane glycoproteins] TCR (T-Cell Receptor) BCR (B-Cell Receptor) Members of the immunoglobulin superfamily Immunogenetics
  • 30. GENES encoding Ig, BCR and TCR: germline organization Cell and Xsome carrying the genes Ig (BCR) Heavy chain locus B-cell, Chromosome # 14 Ig (BCR) Light chain locus B-cell, Xsome # 2 (k), 22 (l) TCR b chain T-cell, Xsome # 7 TCR a chain T-cell, Xsome # 14 MHC class I genes All nucleated Xsome # 6 MHC class II genes APC, Xsome # 6
  • 33. Antibody Molecules • The molecule has a "Y" shape, with the two ends of the fork • 2 heavy chains plus 2 light chains, joined together by disulfide bridges. • Variable (V) regions form antigen binding sites which specifically bind particular antigens • Each Ab molecule has 2 identical Ag binding regions, and thus the Ab molecules can bind together large groups of Ag's.
  • 34. • Each light (L) chain has 2 domains, a variable (V) region and a constant (C) region. – There are only a small number of C regions in each person, but there are very many different V regions. – Note that the V and C regions are together on the same polypeptide chain! • Each heavy (H) chain has 4 domains, a V domain followed by 3 C domains. • The C domains determine the 5 classes of antibodies: IgM (early response), IgG (main blood Ig), IgA (in body secretions), IgE (allergic response), and IgD (mostly a cell surface molecule in the early response). • In many cases, the constant class-specific regions of the H chains bind to receptors on the surface of specific cells. For instance, IgA binds to secretory cells so it gets secreted into tears, mucus, etc. Antibody Molecules
  • 35. • Genes for immunoglobulin (antibodies) – Expression of genes for Ig occurs in B-cells – Antibody genes are composed of segments – Gene of Ig heavy chain …chromosome 14 – Genes for Ig kappa and lambda on chromosome 2 and 22 respectively Antibody Molecules
  • 36. BCR genetics D-diversity, J-joining, V-variability, C-constant Chromosome 14
  • 37. – During B-cell maturation in the bone marrow, Ig gene segments are rearranged and generated into more than 1010 combinations of V region. – Each B cell has a unique combination and is antigenically committed to a specific epitope. – After antigenic stimulation, further rearrangement of C-region gene segments can generate changes in isotypes without changing the specificity of Ig. – Genomic rearrangement is an essential feature of lymphocyte differentiation, and no other vertebrate cell type has been shown to undergo this process. Antibody Molecules
  • 38. Generation of diversity • Antigens – 1011 (100 billion) • Mechanisms – before and after contact with antigen  V(D)J recombination  Junctional diversity  Combinations of receptor chains  Somatic hypermutation (affinity maturation)
  • 39. TCR genetics chain chromosome V D J C α 14 50 - 70 1 β 7 57 2 13 2
  • 40. Major Histocompatibility Complex (MHC) • The MHC is a closely linked complex of genes that govern production of histocompatibility between individuals and species. • In humans, MHC resides on the short arm of chromosome 6 • Class I MHC (HLA) proteins are coded in 3 genes (HLA-A, HLA-B, HLA-C) • Class II MHC (HLA-D) proteins are code in several loci (DP, DQ and DR) • HLA genes are very diverse (polymorphic) i.e. there are many alleles of the class I and II genes
  • 41. MHC Molecules • Between the class I and class II gene loci, there is a third locus (Class III) • This locus contains genes encoding tumor necrosis factor, lymphotoxin and two complement components (C2 and C4) • Class III antigens do not participate in MHC restriction or graft rejection
  • 43. Location and components Class I MHC Class II MHC RBCs Professional APCs Nucleated cells A, B, C DP, DQ, DR Class III codes for other proteins eg complement components, cytokines
  • 44. Class I MHC • α chain (43kDa), β2 microglobulin (12 kDa) • β2-microglobulin – genes on chromosome 15 • Can accommodate 10 amino acids b2-M a-chain Peptide
  • 45. Class II MHC a-chain b-chain Peptide • α chain (34kDa), β chain (29 kDa) • Can accommodate ~15 amino acids
  • 46. Class I MHC and Class II MHC MHC Class I MHC Class II Nomenclature HLA-A, HLA-B, HLA-C HLA-DP, HLA-DQ, HLA-DR Found on All nucleated somatic cells Macrophages, B-cells, Dentritic cells, langerhans cells of skin and activated T cells Recognized by CD8 TC cells CD4 TH cells Functions Presentation of Ag to TC cells leading to elimination of tumor or infected host cell Presentation of Ag to TH cells which secrete cytokines
  • 48. Application of HLA in medicine Transplantation Forensic medicine Anthropological studies Regulating immune responses Disease association
  • 49. Talk Agenda 1. Definition of immunogenetics 2. Basic of immune responses o Innate immunity o Adaptive immunity 3. Diversity for specificity o BCR o TCR o HLA 4. Diseases associated with immunodeficiency
  • 50. impaired function of the immune system (immunodeficiency) resulting in increased susceptibility to infection. IMMUNODEFICIENCY Primary immunodeficiency-PID intrinsic defect of a component of the immune Most by defects in single genes and are hence heritable.. rare Secondary or acquired secondary to another pathological condition, which adversely affects immune function,
  • 52. From a clinical perspective, immuno- deficiencies can be classified into eight categories
  • 53. T AND B CELL IMMUNODEFICIENCIES Next slide
  • 54. SCID; CLASSIFICATION About 15 percent of SCID cases are caused by deficiency of adenosine deaminase (ADA), an enzyme required for the salvage of nucleotides within lymphoid cells. The lack of ADA causes the accumulation of toxic metabolites of adenosine (deoxy- adenosine and deoxy-ATP) within lymphoid cells, resulting in their demise. NO STEM CELLS
  • 55. Mutations of the tyro-sine phosphatase, CD45, which helps to initiate signaling by the TCR, results in T−B+ SCID in humans. Mutation of components of CD3-complex (CD3 γ, ε, and δ) result in a SCID phenotype. During signal transduction via TCRs, the protein tyrosine kinases Lck and ZAP70 are required for phosphorylation of ITAMs on the intracy- toplasmic segment of the TCR. Deficiency of either of these kinases results in rare forms of SCID.
  • 56. T AND B CELL IMMUNODEFICIENCIES
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  • 59. Defects in Leucocyte Migration protein lymphocyte function-associated antigen-1(LFA-1) LFA- 1 expressed on the leucocyte surface and its ligand intercellular adhesion molecule- 1 (ICAM-1) expressed on the luminal surface of activated endothelial cells. •a common β chain (CD18) with three separate α chains called CD11a, b, and c. •CD18-CD11a heterodimers form LFA-1, LAD1 n LAD2
  • 60.  CD18/CD11b Heterodimers form complement receptor 3, (CR3)  CD18 combined to CD11c forms complement receptor 4 (CR4). Mutation of the gene encoding CD18 (resulting in the lack of expression of LFA-1, CR3, and CR4) results in an inherited primary immunodeficiency called leukocyte adhesion deficiency type 1(LAD1). sialyl LewisX, which is expressed on the surface of leucocytes, LAD1 LAD2
  • 62. Ab switch, memory b cells, somatic hypermutation, dendritic cells to prime t cells,CD80 n 86 upregulation HYPER IgM SYNDROMES