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Cells of the immune system ppt

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Gloria Okenze
Gloria Okenze

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Offor, Gloria Nwabugwu Biochemistry programme, Covenant University. Lecturer: Dr. A.H. Adebayo CELLS OFTHE IMMUNE SYSTEM: PHYSIOLOGY, BIOCHEMICAL IMPLICATIONS, AND PATHOPHYSIOLOGY
Outline  Introduction  Formation of blood cells  Types of leucocytes  Cells of the innate immune system  Phagocytosis and intracellular killing  Cells of the adaptive immune system  Cell-Mediated Cytotoxicity  Immunopathology  Conclusion  References
Presentation Objectives  To identify cell types involved in the innate and adaptive immune response.  To highlight the mechanism of combating infection/disease (killing pathogens).  To identify the consequences of alteration in function of the immune cells.
Introduction  White blood cells or leucocytes serve as sentinels and defenders against infection.  They move around the body via the lymphatic and blood circulatory systems.  Leucocytes are classified by morphology- number of nuclei lobes and presence or absence of cytoplasmic granules.  Leukocytes may be found as individual cells throughout the body, as accumulations within lymphoid organs (e.g., spleen, lymph nodes) and at sites of infection or inflammation.  Knowledge of the role that each leukocyte plays is important to
Formation of blood cells  All bloodborne cells originate in the bone marrow.  Pluripotent hematopoietic stem cell in the bone marrow give rise to two major lineages; a myeloid lineage and a lymphoid lineage.  Cells of the myeloid lineage differentiate further into platelets, erythrocytes, eosinophils, basophils (and mast cells), neutrophils, monocytes/macrophages, and some dendritic cells.  Cells of the lymphoid lineage differentiate further into T and B lymphocytes, NK cells, and some
Fig 1: Hematopoiesis
Types of leucocytes  White blood cells that have multilobed nuclei and contain conspicuous cytoplasmic granules are known as granulocytes .  Others with a single, unlobed nucleus and cytoplasm that contains few or no granules are known as agranular leukocytes.  Agranular leukocytes derive from lymphoid or myeloid lineage precursors and account for approximately 35% to 38% of the leukocytes in
Fig 2: Types of leukocytes.
Cells of the innate immune system  Myeloid Cells: First line of defense against invading organisms in non-specific innate immunity. Neutrophils Eosinophils Basophils/Mast cells Monocytes/Macrophages/Dendritic Cells  Lymphoid Cells:
Neutrophils  Comprises approximately 60% of the peripheral blood leukocytes, neutrophils are the most numerous leukocyte population. – Neutrophils have multi lobed nuclei (2-5) and cytoplasmic granules that stain with both acid and basic dyes. – often called polymorphonuclear cells (PMN's).  The neutrophil's main role is in inflammation. – First to arrive at inflammation site – Leave blood/endothelium into tissue (extravasation).  Neutrophils are attracted into the tissue by chemotactic factors stimulated by tissue damage – complement proteins, clotting proteins and T cell derived
 In the tissues, neutrophils are active phagocytes.  They destroy ingested microorganisms via oxygen-dependent or independent pathways.  Produce myeloperoxidases to assist oxidated antimicrobial effects.  Produce lactoferrin and lysozyme as direct antimicrobial agents.  Produce leukotrienes and prostaglandins, products of the lipoxygenase and cyclo-oxygenase pathways, to mediate vascular functions.  Deficiencies in pathways increase susceptibility to infections.
Characteristics of Neutrophil granules Primary granules Secondary granules Azurophilic; young neutrophils Specific for mature neutrophils Contain: cationic proteins, lysozyme, defensins, elastase and Contain: Lysozyme, NADPH oxidase components and myeloperoxidase Lactoferrin and B12-binding protein
Eosinophils  Eosinophils have bilobed nuclei and cytoplasmic granules that stain with the acid dye eosin (hence its name). Constitute 1%-3% of circulating leucocytes.  Involved in asthma.  Eosinophils are motile, sometimes phagocytic, and are particularly active in parasitic infection.
Basophils  Basophils have bilobed nuclei and cytoplasmic granules that stain with the basic dye methylene blue.  Found in low numbers in the blood (<1%). Act like mast cells.  They are nonphagocytic  Involved in allergic reactions (Type I hypersensitivity responses).  Have high affinity Fc receptors for IgE on their surface.  When an individual is exposed to an allergen, specific IgE is produced. This IgE binds to the surface of basophils.  Upon re-exposure to the allergen, the allergen binds to IgE on the surface of basophils resulting in degranulation.  Cross-linking of the IgE causes the basophils to release pharmacologically active mediators
Mast cells  Similar importance in allergic reactions as basophils, but only found in tissues.  Contain granules with preformed mediators to be released after stimulation – histamine, prostaglandins – leukotrienes  Stimulation of mast cells occurs by the anaphylatoxins (complement proteins C3a and C5a) or by cross-linking of surface immunoglobulin (IgE).
Monocytes/Macrophages  Circulate in the blood after leaving the bone marrow.  Survive only a day or so before they enter the tissue to mature into macrophages.  Involved in phagocytosis and intracellular killing of microorganisms.  Generation of toxic metabolites through respiratory burst.  Production of nitric oxide, hydrogen peroxide, superoxide anion.  Monocytes/Macrophages are antigen processing and presenting cells.  Degrative enzymes in lysosomal granules.  Chew ingested proteins.  Present to adaptive cells.
Macrophages  When monocytes enter the tissues and become macrophages: – Enlarge and increase production of intracellular lysozymes – Greater phagocytosis. – Can live for years in tissue; highly motile.  Activation of these cells occurs by phagocytosis of antigens, or in response to T cell derived cytokines.  Activated macrophages recognize and remove unwanted particulate matter including products
 After activation, these cells secrete cytokines, chemokines, lysozymes and other factors to upregulate immune response. In chronic inflammation, macrophage scavengers can become “giant cells” or “foamy macrophages”. Fig: Electron micrograph of macrophag
Dendritic cells  Specialized phagocytic cells found in most tissues.  Arise both from the myeloid and lymphoid lineages.  Abundant at interfaces between the external and internal environments (skin, lining of the gastrointestinal tract), where they encounter invading pathogens.  Actively motile; continuously sample surroundings by endocytic processes.  Dendritic cells are very efficient at activation of T cells.
Natural Killer cells  Also known as large granular lymphocytes (LGLs)  Functionally cytotoxic representing an innate population that kill virally infected or tumor target cells.  Killing is nonspecific - they do not need to recognize foreign antigens presented on the target cell. – NK cells do not have a specific cell receptor. Target recognition occurs by a Killer Inhibitory Receptor, KIR, which assess MHC I molecules on the target cell surface. MHC 1 molecule is lacking on infected and tumor targets.  Kill targets by releasing perforin which damages target cell membranes. Can also induce apoptosis in the target cell.  NK cells is different from NK T cells. -NKT cells has some of the attributes of T cell and NK cell. Like T cells, NK1-T cells have T cell receptors (TCRs).Unlike most T cells, the TCRs of NK1-T cells interact with MHC-like molecules called CD1 rather than with class I or class II MHC molecules. Like NK cells, they have variable levels of CD16 and other receptors typical of NK
Phagocytosis and intracellular killing  Phagocytosis is the engulfment and degradation of microbes and other particulate matter by cells such as macrophages/monocytes, dend ritic cells, and neutrophils .  Steps in phagocytosis- 1) Detection of the foreign particle and movement of the phagocyte to the area by chemotaxis. 2) Attachment of the foreign particle to the phagocyte. 3) Engulfment or ingestion of the foreign particle into a vesicle called a phagosome. 4) Fusion with lysosome and formation of the phagolysosome. 5) Intracellular killing and digestion. 6) In the case of macrophages, egestion and antigen presentation.  Phagocytes detect microbes by the presence of N-formylated peptides, activated complement proteins and the mediators of inflammation.  Phagocytes attach to microbes using opsonins, such as IgG and the complement protein C3b. In the absence of opsonins, phagocytes can
Fig: Steps in phagocytosis
Pathways of intracellular killing  Lysosomes employ multiple mechanisms for killing and degrading ingested microbe. These include;  Oxygen-independent killing  Oxygen-dependent-MPO independent killing  Oxygen-dependent-MPO dependent killing  Nitric Oxide mediated killing  In oxygen-independent killing, activated phagocytes synthesize lysozyme and various hydrolytic enzymes whose degradative activities do not require oxygen.
Mediators of oxygen-independent killing in phagolysosome  During phagocytosis there is an increase in glucose and oxygen consumption which is referred to as the respiratory burst.  The consequence of the respiratory burst is that a number of oxygen-containing compounds are produced which kill the bacteria being phagocytosed. This is referred to as oxygen- Effector Molecule Function Cationic proteins (cathepsin) Damage to microbial membranes Lysozyme Hydrolyses mucopeptides in the cell wall Lactoferrin Deprives pathogens of iron Hydrolytic enzymes (proteases) Digests killed organisms
Oxygen-dependent myeloperoxidase- independent reactions
Oxygen-dependent myeloperoxidase- dependent reactions Detoxification reactions
Nitric oxide-dependent killing  Once microorganisms are destroyed, the unwanted organic material is expelled from the cell in a process called egestion.  Egestion is the opposite of ingestion and the molecular mechanism is basically the reverse of phagocytosis with the microbial leftovers being dumped into the blood and lymph.  Some of this microbial debris are not egested, but binds to special protein complexes (called Major Histocompatibility Complex molecules) on the membranes of macrophages
Cells of the adaptive immune system  Adaptive immune responses are mediated by a specialized group of leukocytes, the lymphocytes, which include T and B lymphocytes (T cells and B cells) that specifically recognize foreign material or antigens.  All lymphocytes are derived from bone marrow stem cells, but T cells then develop in the thymus, while B cells develop in the bone
B Lymphocytes  Develop from stem cells in the bone marrow.  Produce antibodies with specificity for antigens and display it on their surfaces to function as BCRs.  Integral in humoral immunity  Plasma cells = terminally differentiated B cells that secrete immunoglobulins.  Memory cells- secondary immune response is swifter and stronger.  Upon activation, a B cell can switch to produce a different class of antibody, with the same antigen specificity.  Activation into antibody secreting cells is antigen- dependent.
T-Lymphocytes  T lymphocytes develop in the thymus.  Regulate immune responses.  Integral in cell mediated immunity.  Critical in B cell-antibody production.  Mature T cells display either CD4 or CD8.  Cells with a CD4 marker are called helper T cells (Th cells).  CD8 marker positive cells are cytotoxic T cells (Tc cells).  There are several different types of T cell, and they have a variety of functions :  Type 1 helper T cells or TH1 cells - interacts with mononuclear phagocytes and helps them destroy intracellular pathogens•  Type 2 helper T cells or TH2 cells; interacts with B cells and helps them to divide, differentiate, and make antibody•  Cytotoxic T lymphocytes (CTLs or TC cells). responsible for the destruction of host cells that have become infected by viruses or other intracellular pathogens.  Regulatory T cells or Tregs, help to control the development of immune responses, and limit reactions against self tissues.
Fig: B and T Lymphocytes
Cell-Mediated Cytotoxicity  Cytotoxicity describes the ways in which leukocytes recognize and destroy other cells.  Cell-mediated cytotoxicity is an essential defense against:  intracellular pathogens, including viruses;  some bacteria;  some parasites.  Tumor cells, eukaryotic pathogens, and even cells of the body may also become the target of cytotoxic cells.  Several types of cell have cytotoxic activity including:  cytotoxic T lymphocytes (CTLs);  natural killer (NK) cells  CTLs and NK cells use a variety of different mechanisms to kill their targets. These include:  direct cell–cell signaling via surface molecules; and  granule-associated killing
Immunopathology  Autoimmune disease - When the immune system reacts against ‘self’ components, for example rheumatoid arthritis or pernicious anemia.  Immunodeficiency- If any elements of the immune system are defective, the individual may not be able to fight infections adequately.  primary immundeficiencies are hereditary and start to manifest shortly after birth; eg chronic granulomatous disease (CGD) and leukocyte adhesion deficiency (LAD).  Secondary immunodeficiencies develop later in life, for example the acquired immune deficiency syndrome (AIDS).  Hypersensitivity- Sometimes immune reactions are out of all proportion to the damage that may be caused by a pathogen. The immune system may also mount a reaction to a harmless antigen, such as a food molecule causing
Table 1. Characteristic infections in primary immunodeficiencies.
Conclusion  The immune system has evolved to protect us from pathogens.  Phagocytes and lymphocytes are key mediators of immunity. Phagocytes internalize pathogens and degrade them. Lymphocytes (B and T cells) have receptors that recognize specific molecular components of pathogens and have specialized functions. B cells make antibodies (effective against extracellular pathogens), cytotoxic T lymphocytes (CTLs) kill virally infected cells, and helper T cells coordinate the immune response by direct cell–cell interactions and the release of cytokines.  The immune system may fail (immunopathology). This can be a result of immunodeficiency, hypersensitivity, or
References  Doan, T., Melvold, R., Viselli, S. and Waltenbaugh, C.(2013). Lippincott’s illustrated reviews Immunology. Philadelphia, 2nd Edn. Lippincott Williams & Wilkins. ISBN 978-1-4511-0937-5.  Kindt, T.J., Osborne, B.A. and Goldsby, R.A. (2006). Kuby Immunology, 6th edn. Oxford: WH Freeman.  Male, D., Brostoff, J., Roth, D.B. and Roitt, I.(2013). Immunology. China, 8th Edn. Elsevier. ISBN 978-0- 702-04548-6.  Roitt, I.M. and Delves, P. (2011)Essential
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Cells of the immune system ppt

  • 1. Offor, Gloria Nwabugwu Biochemistry programme, Covenant University. Lecturer: Dr. A.H. Adebayo CELLS OFTHE IMMUNE SYSTEM: PHYSIOLOGY, BIOCHEMICAL IMPLICATIONS, AND PATHOPHYSIOLOGY
  • 2. Outline  Introduction  Formation of blood cells  Types of leucocytes  Cells of the innate immune system  Phagocytosis and intracellular killing  Cells of the adaptive immune system  Cell-Mediated Cytotoxicity  Immunopathology  Conclusion  References
  • 3. Presentation Objectives  To identify cell types involved in the innate and adaptive immune response.  To highlight the mechanism of combating infection/disease (killing pathogens).  To identify the consequences of alteration in function of the immune cells.
  • 4. Introduction  White blood cells or leucocytes serve as sentinels and defenders against infection.  They move around the body via the lymphatic and blood circulatory systems.  Leucocytes are classified by morphology- number of nuclei lobes and presence or absence of cytoplasmic granules.  Leukocytes may be found as individual cells throughout the body, as accumulations within lymphoid organs (e.g., spleen, lymph nodes) and at sites of infection or inflammation.  Knowledge of the role that each leukocyte plays is important to
  • 5. Formation of blood cells  All bloodborne cells originate in the bone marrow.  Pluripotent hematopoietic stem cell in the bone marrow give rise to two major lineages; a myeloid lineage and a lymphoid lineage.  Cells of the myeloid lineage differentiate further into platelets, erythrocytes, eosinophils, basophils (and mast cells), neutrophils, monocytes/macrophages, and some dendritic cells.  Cells of the lymphoid lineage differentiate further into T and B lymphocytes, NK cells, and some
  • 7. Types of leucocytes  White blood cells that have multilobed nuclei and contain conspicuous cytoplasmic granules are known as granulocytes .  Others with a single, unlobed nucleus and cytoplasm that contains few or no granules are known as agranular leukocytes.  Agranular leukocytes derive from lymphoid or myeloid lineage precursors and account for approximately 35% to 38% of the leukocytes in
  • 8. Fig 2: Types of leukocytes.
  • 9. Cells of the innate immune system  Myeloid Cells: First line of defense against invading organisms in non-specific innate immunity. Neutrophils Eosinophils Basophils/Mast cells Monocytes/Macrophages/Dendritic Cells  Lymphoid Cells:
  • 10. Neutrophils  Comprises approximately 60% of the peripheral blood leukocytes, neutrophils are the most numerous leukocyte population. – Neutrophils have multi lobed nuclei (2-5) and cytoplasmic granules that stain with both acid and basic dyes. – often called polymorphonuclear cells (PMN's).  The neutrophil's main role is in inflammation. – First to arrive at inflammation site – Leave blood/endothelium into tissue (extravasation).  Neutrophils are attracted into the tissue by chemotactic factors stimulated by tissue damage – complement proteins, clotting proteins and T cell derived
  • 11.  In the tissues, neutrophils are active phagocytes.  They destroy ingested microorganisms via oxygen-dependent or independent pathways.  Produce myeloperoxidases to assist oxidated antimicrobial effects.  Produce lactoferrin and lysozyme as direct antimicrobial agents.  Produce leukotrienes and prostaglandins, products of the lipoxygenase and cyclo-oxygenase pathways, to mediate vascular functions.  Deficiencies in pathways increase susceptibility to infections.
  • 12. Characteristics of Neutrophil granules Primary granules Secondary granules Azurophilic; young neutrophils Specific for mature neutrophils Contain: cationic proteins, lysozyme, defensins, elastase and Contain: Lysozyme, NADPH oxidase components and myeloperoxidase Lactoferrin and B12-binding protein
  • 13. Eosinophils  Eosinophils have bilobed nuclei and cytoplasmic granules that stain with the acid dye eosin (hence its name). Constitute 1%-3% of circulating leucocytes.  Involved in asthma.  Eosinophils are motile, sometimes phagocytic, and are particularly active in parasitic infection.
  • 14. Basophils  Basophils have bilobed nuclei and cytoplasmic granules that stain with the basic dye methylene blue.  Found in low numbers in the blood (<1%). Act like mast cells.  They are nonphagocytic  Involved in allergic reactions (Type I hypersensitivity responses).  Have high affinity Fc receptors for IgE on their surface.  When an individual is exposed to an allergen, specific IgE is produced. This IgE binds to the surface of basophils.  Upon re-exposure to the allergen, the allergen binds to IgE on the surface of basophils resulting in degranulation.  Cross-linking of the IgE causes the basophils to release pharmacologically active mediators
  • 15. Mast cells  Similar importance in allergic reactions as basophils, but only found in tissues.  Contain granules with preformed mediators to be released after stimulation – histamine, prostaglandins – leukotrienes  Stimulation of mast cells occurs by the anaphylatoxins (complement proteins C3a and C5a) or by cross-linking of surface immunoglobulin (IgE).
  • 16. Monocytes/Macrophages  Circulate in the blood after leaving the bone marrow.  Survive only a day or so before they enter the tissue to mature into macrophages.  Involved in phagocytosis and intracellular killing of microorganisms.  Generation of toxic metabolites through respiratory burst.  Production of nitric oxide, hydrogen peroxide, superoxide anion.  Monocytes/Macrophages are antigen processing and presenting cells.  Degrative enzymes in lysosomal granules.  Chew ingested proteins.  Present to adaptive cells.
  • 17. Macrophages  When monocytes enter the tissues and become macrophages: – Enlarge and increase production of intracellular lysozymes – Greater phagocytosis. – Can live for years in tissue; highly motile.  Activation of these cells occurs by phagocytosis of antigens, or in response to T cell derived cytokines.  Activated macrophages recognize and remove unwanted particulate matter including products
  • 18.  After activation, these cells secrete cytokines, chemokines, lysozymes and other factors to upregulate immune response. In chronic inflammation, macrophage scavengers can become “giant cells” or “foamy macrophages”. Fig: Electron micrograph of macrophag
  • 19. Dendritic cells  Specialized phagocytic cells found in most tissues.  Arise both from the myeloid and lymphoid lineages.  Abundant at interfaces between the external and internal environments (skin, lining of the gastrointestinal tract), where they encounter invading pathogens.  Actively motile; continuously sample surroundings by endocytic processes.  Dendritic cells are very efficient at activation of T cells.
  • 20. Natural Killer cells  Also known as large granular lymphocytes (LGLs)  Functionally cytotoxic representing an innate population that kill virally infected or tumor target cells.  Killing is nonspecific - they do not need to recognize foreign antigens presented on the target cell. – NK cells do not have a specific cell receptor. Target recognition occurs by a Killer Inhibitory Receptor, KIR, which assess MHC I molecules on the target cell surface. MHC 1 molecule is lacking on infected and tumor targets.  Kill targets by releasing perforin which damages target cell membranes. Can also induce apoptosis in the target cell.  NK cells is different from NK T cells. -NKT cells has some of the attributes of T cell and NK cell. Like T cells, NK1-T cells have T cell receptors (TCRs).Unlike most T cells, the TCRs of NK1-T cells interact with MHC-like molecules called CD1 rather than with class I or class II MHC molecules. Like NK cells, they have variable levels of CD16 and other receptors typical of NK
  • 21. Phagocytosis and intracellular killing  Phagocytosis is the engulfment and degradation of microbes and other particulate matter by cells such as macrophages/monocytes, dend ritic cells, and neutrophils .  Steps in phagocytosis- 1) Detection of the foreign particle and movement of the phagocyte to the area by chemotaxis. 2) Attachment of the foreign particle to the phagocyte. 3) Engulfment or ingestion of the foreign particle into a vesicle called a phagosome. 4) Fusion with lysosome and formation of the phagolysosome. 5) Intracellular killing and digestion. 6) In the case of macrophages, egestion and antigen presentation.  Phagocytes detect microbes by the presence of N-formylated peptides, activated complement proteins and the mediators of inflammation.  Phagocytes attach to microbes using opsonins, such as IgG and the complement protein C3b. In the absence of opsonins, phagocytes can
  • 22. Fig: Steps in phagocytosis
  • 23. Pathways of intracellular killing  Lysosomes employ multiple mechanisms for killing and degrading ingested microbe. These include;  Oxygen-independent killing  Oxygen-dependent-MPO independent killing  Oxygen-dependent-MPO dependent killing  Nitric Oxide mediated killing  In oxygen-independent killing, activated phagocytes synthesize lysozyme and various hydrolytic enzymes whose degradative activities do not require oxygen.
  • 24. Mediators of oxygen-independent killing in phagolysosome  During phagocytosis there is an increase in glucose and oxygen consumption which is referred to as the respiratory burst.  The consequence of the respiratory burst is that a number of oxygen-containing compounds are produced which kill the bacteria being phagocytosed. This is referred to as oxygen- Effector Molecule Function Cationic proteins (cathepsin) Damage to microbial membranes Lysozyme Hydrolyses mucopeptides in the cell wall Lactoferrin Deprives pathogens of iron Hydrolytic enzymes (proteases) Digests killed organisms
  • 27. Nitric oxide-dependent killing  Once microorganisms are destroyed, the unwanted organic material is expelled from the cell in a process called egestion.  Egestion is the opposite of ingestion and the molecular mechanism is basically the reverse of phagocytosis with the microbial leftovers being dumped into the blood and lymph.  Some of this microbial debris are not egested, but binds to special protein complexes (called Major Histocompatibility Complex molecules) on the membranes of macrophages
  • 28. Cells of the adaptive immune system  Adaptive immune responses are mediated by a specialized group of leukocytes, the lymphocytes, which include T and B lymphocytes (T cells and B cells) that specifically recognize foreign material or antigens.  All lymphocytes are derived from bone marrow stem cells, but T cells then develop in the thymus, while B cells develop in the bone
  • 29. B Lymphocytes  Develop from stem cells in the bone marrow.  Produce antibodies with specificity for antigens and display it on their surfaces to function as BCRs.  Integral in humoral immunity  Plasma cells = terminally differentiated B cells that secrete immunoglobulins.  Memory cells- secondary immune response is swifter and stronger.  Upon activation, a B cell can switch to produce a different class of antibody, with the same antigen specificity.  Activation into antibody secreting cells is antigen- dependent.
  • 30. T-Lymphocytes  T lymphocytes develop in the thymus.  Regulate immune responses.  Integral in cell mediated immunity.  Critical in B cell-antibody production.  Mature T cells display either CD4 or CD8.  Cells with a CD4 marker are called helper T cells (Th cells).  CD8 marker positive cells are cytotoxic T cells (Tc cells).  There are several different types of T cell, and they have a variety of functions :  Type 1 helper T cells or TH1 cells - interacts with mononuclear phagocytes and helps them destroy intracellular pathogens•  Type 2 helper T cells or TH2 cells; interacts with B cells and helps them to divide, differentiate, and make antibody•  Cytotoxic T lymphocytes (CTLs or TC cells). responsible for the destruction of host cells that have become infected by viruses or other intracellular pathogens.  Regulatory T cells or Tregs, help to control the development of immune responses, and limit reactions against self tissues.
  • 31. Fig: B and T Lymphocytes
  • 32. Cell-Mediated Cytotoxicity  Cytotoxicity describes the ways in which leukocytes recognize and destroy other cells.  Cell-mediated cytotoxicity is an essential defense against:  intracellular pathogens, including viruses;  some bacteria;  some parasites.  Tumor cells, eukaryotic pathogens, and even cells of the body may also become the target of cytotoxic cells.  Several types of cell have cytotoxic activity including:  cytotoxic T lymphocytes (CTLs);  natural killer (NK) cells  CTLs and NK cells use a variety of different mechanisms to kill their targets. These include:  direct cell–cell signaling via surface molecules; and  granule-associated killing
  • 33.
  • 34. Immunopathology  Autoimmune disease - When the immune system reacts against ‘self’ components, for example rheumatoid arthritis or pernicious anemia.  Immunodeficiency- If any elements of the immune system are defective, the individual may not be able to fight infections adequately.  primary immundeficiencies are hereditary and start to manifest shortly after birth; eg chronic granulomatous disease (CGD) and leukocyte adhesion deficiency (LAD).  Secondary immunodeficiencies develop later in life, for example the acquired immune deficiency syndrome (AIDS).  Hypersensitivity- Sometimes immune reactions are out of all proportion to the damage that may be caused by a pathogen. The immune system may also mount a reaction to a harmless antigen, such as a food molecule causing
  • 35. Table 1. Characteristic infections in primary immunodeficiencies.
  • 36. Conclusion  The immune system has evolved to protect us from pathogens.  Phagocytes and lymphocytes are key mediators of immunity. Phagocytes internalize pathogens and degrade them. Lymphocytes (B and T cells) have receptors that recognize specific molecular components of pathogens and have specialized functions. B cells make antibodies (effective against extracellular pathogens), cytotoxic T lymphocytes (CTLs) kill virally infected cells, and helper T cells coordinate the immune response by direct cell–cell interactions and the release of cytokines.  The immune system may fail (immunopathology). This can be a result of immunodeficiency, hypersensitivity, or
  • 37. References  Doan, T., Melvold, R., Viselli, S. and Waltenbaugh, C.(2013). Lippincott’s illustrated reviews Immunology. Philadelphia, 2nd Edn. Lippincott Williams & Wilkins. ISBN 978-1-4511-0937-5.  Kindt, T.J., Osborne, B.A. and Goldsby, R.A. (2006). Kuby Immunology, 6th edn. Oxford: WH Freeman.  Male, D., Brostoff, J., Roth, D.B. and Roitt, I.(2013). Immunology. China, 8th Edn. Elsevier. ISBN 978-0- 702-04548-6.  Roitt, I.M. and Delves, P. (2011)Essential