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Immunity to Infectious Diseases

0. Immunity to Infectious Diseases. BIOS 486A/586A K.J.Goodrum 2006. 0. Topic Outline. Routes and sites of infection Mechanisms of tissue injury in infection Timing of immune responses to infection Regulation of cell-mediated (T H 1) vs. humoral immunity (T H 2) in infections

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Immunity to Infectious Diseases

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  1. 0 Immunity to Infectious Diseases BIOS 486A/586A K.J.Goodrum 2006

  2. 0 Topic Outline • Routes and sites of infection • Mechanisms of tissue injury in infection • Timing of immune responses to infection • Regulation of cell-mediated (TH1) vs. humoral immunity (TH2) in infections • Effector mechanisms for immunity to different pathogens • Microbial evasion of immune responses • Immunizations/vaccines

  3. 0 Routes and sites of infection

  4. 0 Primary Route of Infection: Microbial Adherence and Invasion of epithelial tissues (lung, gut, other) Janeway, Fig. 10.2

  5. 0 Primary Route of Infection: Microbial Adherence and Invasion of epithelial tissues (continued). Janeway, Fig. 10.2

  6. 0 Janeway. Fig. 10.4. Infection compartments

  7. 0 Mechanisms of tissue injury in infection

  8. 0 Janeway. Fig. 10.5. Mechanisms of Pathogen-induced tissue Damage

  9. 0 Janeway. Fig. 10.5. Mechanisms of Pathogen-induced tissue Damage (continued)

  10. 0 Timing of immune responses to infection

  11. 0 Janeway. Fig. 10.1. Time course of immune response to acute infection.

  12. 0 Regulation of cell-mediated (TH1) vs. humoral immunity (TH2) in infections

  13. 0 Janeway. Fig.10.9. Infection induced Th1 vs. Th2 responses.

  14. 0 Janeway. Fig. 11.6. The effect of T helper subpopulations on leprosy outcome.

  15. 0 Janeway. Fig. 11.6. The effect of T helper subpopulations on leprosy outcome. (continued)

  16. 0 Effector mechanisms for immunity to different pathogens

  17. 0 Janeway. Fig. 10.17. Protective Effector Mechanisms against various infectious microbes

  18. 0 Janeway. Fig. 10.17. Protective Effector Mechanisms against various infectious microbes (continued)

  19. 0 Janeway. Fig. 10.17. Protective Effector Mechanisms against various infectious microbes (continued)

  20. 0 Janeway. Fig. 10.23. Mucosal gdT cell function.

  21. 0 Janeway. Fig. 10.24. Mucosal Secretory IgA function

  22. 0 Janeway. Fig. 10.27. Recognition of intracellular infection by Nod1.

  23. 0 Janeway. Fig. 10.27. Recognition of intracellular infection by Nod1.(continued)

  24. 0 Janeway. Fig. 2.5. Innate recognition of microbes and phagocytosis by macrophages

  25. 0 Janeway. Fig. 2.18. Microbial activation of complement pathways for inflammation.

  26. 0 Janeway. Fig. 9.1. Protective effector mechanisms of antibody.

  27. 0 Janeway. Fig. 1.24 Protective effector mechanisms of antibody.

  28. 0 Janeway. Fig. 8.27. Effector T cell populations and effector mechanisms.

  29. 0 Microbial evasion of immune responses

  30. 0 Janeway. Fig. 11.1. Immune evasion via multiple antigenic variants of microbes (serotypes).

  31. 0 Fig.11.1 continued

  32. 0 Fig. 11.1 continued

  33. 0 Janeway. Fig. 11.2. Immune Evasion via antigen drift/shift.

  34. 0 Janeway. Fig. 11.2. Immune Evasion via antigen drift/shift. (continued)

  35. 0 Janeway. Fig. 11.3. Immune evasion via sequential DNA rearrangements of microbial antigens.

  36. 0 Janeway. Fig. 11.3. Immune evasion via sequential DNA rearrangements of microbial antigens. (continued)

  37. 0 Janeway. Fig. 11.5. Immune evasion mechanisms of herpes viruses.

  38. 0 Janeway. Fig. 11.5. Immune evasion mechanisms of herpes viruses. (continued)

  39. 0 Janeway. Fig. 11.5. Immune evasion mechanisms of herpes viruses. (continued)

  40. 0 Immunizations/vaccines

  41. 0 Janeway. Fig. 14.21. Childhood vaccination schedule in USA.

  42. 0 Janeway. Fig. 14.23.

  43. 0 Janeway. Fig. 14.23. continued.

  44. 0 Summary • Immunity to infection depends on a combination of innate mechanisms (phagocytosis, complement, etc.) and antigen specific adaptive responses (antibody, effector T lymphocytes). • The immune system regulates which specific responses predominate (humoral vs. cell-mediated) based on the body compartment infected (intracellular vs. extracellular) and on cytokine signals present at initial antigen contact (Th1 vs. Th2 responses).

  45. 0 Summary-continued • Disease-causing microbes have virulence mechanisms that resist or evade innate and/or specific immune effector functions. • Recovery from natural infection or artificial immunization promote specific longterm immunity to re-infection (immunological memory).

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