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Fever Slide 12.23 Abnormally high body temperature Hypothalmus heat regulation can be reset by pyrogens (secreted by white blood cells) High temperatures inhibit the release of iron and zinc from liver and spleen needed by bacteria Fever also increases the speed of tissue repair Causes protein denaturation
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Specific Defense: The Immune System – Third Line of Defense Slide 12.24 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Antigen specific – recognizes and acts against particular foreign substances Systemic – not restricted to the initial infection site Has memory – recognizes and mounts a stronger attack on previously encountered pathogens
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Types of Immunity Slide 12.25 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Humoral immunity (B cells) Antibody-mediated immunity Cells produce chemicals for defense Incorporates protein complement system Cellular immunity (T cells) Cell-mediated immunity Cells target virus infected cells
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Antigens Slide 12.26 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Any substance capable of exciting the immune system and provoking an immune response Examples of common antigens Foreign proteins Nucleic acids Large carbohydrates Some lipids Pollen grains Microorganisms
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Self-Antigens Slide 12.27 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Human cells have many surface proteins Our immune cells do not attack our own proteins Our cells in another person’s body can trigger an immune response because they are foreign Restricts donors for transplants
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Allergies Slide 12.28 Many small molecules (called haptens or incomplete antigens) are not antigenic, but link up with our own proteins The immune system may recognize and respond to a protein-hapten combination The immune response is harmful rather than protective because it attacks our own cells (cells that have formed protein-hapten complex)
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Cells of the Immune System Slide 12.29 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Lymphocytes Originate from hemocytoblasts in the red bone marrow B lymphocytes become immunocompetent in the bone marrow T lymphocytes become immunocompetent in the thymus Macrophages Arise from monocytes Become widely distributed in lymphoid organs
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Activation of Lymphocytes Slide 12.30 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.9
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Humoral (Antibody-Mediated) Immune Response Slide 12.31a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings B lymphocytes with specific receptors bind to a specific antigen The binding event activates the lymphocyte to undergo clonal selection A large number of (B) clones are produced (primary humoral response)
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Humoral (Antibody Mediated) Immune Response Slide 12.31b Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Most B cells become plasma cells Produce antibodies to destroy antigens Activity lasts for four or five days Some B cells become long-lived memory cells (secondary humoral response)
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Humoral Immune Response Slide 12.32 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.10
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Secondary Response Slide 12.33 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Memory cells are long-lived A second exposure causes a rapid response The secondary response is stronger and longer lasting Figure 12.11
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Active Immunity Slide 12.34 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Your B cells encounter antigens and produce antibodies Active immunity can be naturally or artificially acquired Figure 12.12
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Passive Immunity Slide 12.35 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Antibodies are obtained from someone else Conferred naturally from a mother to her fetus Conferred artificially from immune serum or gamma globulin Immunological memory does not occur Protection provided by “borrowed antibodies”
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Monoclonal Antibodies Slide 12.36 Antibodies prepared for clinical testing or diagnostic services Produced from descendents of a single cell line (clones produced from 1 original cell) Can be produced for any antigen Examples of uses for monoclonal antibodies Diagnosis of pregnancy Treatment after exposure to hepatitis and rabies
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Antibodies (Immunoglobulins) (Igs) Slide 12.37 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Soluble proteins secreted by B cells (plasma cells) Carried in blood plasma Capable of binding specifically to an antigen
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Antibody Structure Slide 12.38a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Four amino acid chains linked by disulfide bonds Two identical amino acid chains are linked to form a heavy chain Figure 12.13b
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Antibody Structure Slide 12.38b The other two identical chains are light chains Specific antigen-binding sites are present Figure 12.13b
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Antibody Classes Slide 12.39 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Antibodies of each class have slightly different roles Five major immunoglobulin classes IgM – can fix complement IgA – found mainly in mucus IgD – important in activation of B cell IgG – can cross the placental barrier IgE – involved in allergies
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Antibody Function Slide 12.40 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Antibodies inactivate antigens in a number of ways Complement fixation Neutralization Agglutination Precipitation
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Antibody Function Slide 12.41 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.14
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Cellular (Cell-Mediated) Immune Response Slide 12.42 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Antigens must be presented by macrophages to an immunocompetent T cell (antigen presentation) T cells must recognize nonself and self (double recognition) After antigen binding, clones form as with B cells, but different classes of cells are produced
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Cellular (Cell-Mediated) Immune Response Slide 12.43 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.15
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T Cell Clones Slide 12.44a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Cytotoxic T cells (used to be called Killer T cells) Specialize in killing infected cells Insert a toxic chemical (perforin) Helper T cells Recruit other cells to fight the invaders Interact directly with B cells
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T Cell Clones Slide 12.44b Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Suppressor T cells (think immune system negative feedback) Release chemicals to suppress the activity of T and B cells Stop the immune response to prevent uncontrolled activity A few members of each clone are memory cells
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Summary of the Immune Response Slide 12.45 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.16
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Organ Transplants and Rejection Slide 12.46a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Major types of grafts Autografts – tissue transplanted from one site to another on the same person Isografts – tissue grafts from an identical person (identical twin) Allografts – tissue taken from an unrelated person Xenografts – tissue taken from a different animal species
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Organ Transplants and Rejection Slide 12.46b Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Autografts and isografts are ideal donors Xenografts are rarely successful Allografts are more successful with a closer tissue match
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Disorders of Immunity: Allergies (Hypersensitivity) Slide 12.47a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Abnormal, vigorous immune responses Types of allergies Immediate hypersensitivity Triggered by release of histamine from IgE binding to mast cells Reactions begin within seconds of contact with allergen Anaphylactic shock – dangerous, systemic response
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Disorders of Immunity: Allergies (Hypersensitivity) Slide 12.47b Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Types of allergies (continued) Delayed hypersensitivity Triggered by the release of lymphokines from activated helper T cells Symptoms usually appear 1–3 days after contact with antigen
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Allergy Mechanisms Slide 12.48 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Figure 12.17
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Disorders of Immunity: Immunodeficiencies Slide 12.49 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Production or function of immune cells or complement is abnormal May be congenital or acquired Includes AIDS – Acquired Immune Deficiency Syndrome
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Disorders of Immunity: Autoimmune Diseases Slide 12.50a Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings The immune system does not distinguish between self and nonself The body produces antibodies and sensitized T lymphocytes that attack its own tissues
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Disorders of Immunity: Autoimmune Diseases Slide 12.50b Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Examples of autoimmune diseases Multiple sclerosis – white matter of brain and spinal cord are destroyed Myasthenia gravis – impairs communication between nerves and skeletal muscles Juvenile diabetes (type I)– destroys pancreatic beta cells that produce insulin Rheumatoid arthritis – destroys joints Systemic lupus erythematosus (SLE) – affects kidney, heart, lung and skin Glomerulonephritis – impairment of renal function
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Developmental Aspects of the Lymphatic System and Body Defenses Slide 12.52 Copyright © 2003 Pearson Education, Inc. publishing as Benjamin Cummings Except for thymus and spleen, the lymphoid organs are poorly developed before birth A newborn has no functioning lymphocytes at birth; only passive immunity from the mother If lymphatics are removed or lost, severe edema results, but vessels grow back in time
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