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Lecture on Innate Immunity and Inflammation

Innate Immunity: An Evolutionary View. All multicellular organisms have defense mechanisms against microbial and viral infectionsFor vertebrates, immune defense can be divided into innate immunity and adaptive immunityVertebrate innate immune elements are closely related to components of immunity

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Lecture on Innate Immunity and Inflammation

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    1. Lecture on Innate Immunity and Inflammation Evolutionary View Epithelial barriers to infection Induction of inflammation by complement and Toll-like receptors Inflammation and recruitment of phagocytes Killing of bacteria by phagocytes Anti-viral innate immunity: the interferon system and apoptosis of virus-infected cells

    2. Innate Immunity: An Evolutionary View All multicellular organisms have defense mechanisms against microbial and viral infections For vertebrates, immune defense can be divided into innate immunity and adaptive immunity Vertebrate innate immune elements are closely related to components of immunity in invertebrates

    3. Innate Immunity: An Evolutionary View All multicellular organisms have defense mechanisms against microbial and viral infections For vertebrates, immune defense can be divided into innate immunity and adaptive immunity Vertebrate innate immune elements are closely related to components of immunity in invertebrates Innate immunity retains importance as A first line of defense, slowing growth of infectious agents until adaptive immunity kicks in A means of directing adaptive immunity (induction of inflammation, activation of dendritic cells, and production of cytokines that specialize immune responses)

    4. Recognition mechanisms of innate immunity Microbes evolve rapidly, so innate immunity must focus on broadly expressed molecules characteristic of broad groups of microbes (“pathogen-associated molecular patterns” PAMPs); “pattern recognition receptors” Molecules recognized tend to be structural elements that are common to broad classes of microbes and are very hard to change (only useful to think of them as “patterns” in some cases)

    5. The Epithelial Layer: The initial barrier to infection Physical barrier of the epithelial layer (toughness of barrier varies by location due to other functions: air exchange, nutrient uptake, etc.) Mucus/cilia to remove particles (lung, intestines) Acid pH of the stomach Anti-microbial peptides secreted by some epithelial cells (small intestines, small airways of lungs) Commensal bacteria (compete with pathogenic bacteria) 6. Secretory IgA (adaptive immunity) 7. Intraepithelial lymphocytes (adaptive immunity)

    6. Anti-Microbial Peptides Made by neutrophils and some epithelial cells (small intestines, small airways) Short, cationic peptides (most 29-35 amino acids long) Interact strongly with acidic phospholipids and thought to form pores in membrane (eucaryotic membranes often have negative charge on carbohydrate rather than on phospholipid of outside of bilayer; may account for greater effect of peptides on microbes ) Differentially active against different micro-organisms (evasion?)

    7. Recognition of an infection once it gets past the epithelial barrier Soluble innate immune recognition elements (collectins, ficolins, complement) Sentinel innate immune cells of tissues: tissue macrophages, mast cells and immature dendritic cells, which induce inflammation (1st two) and trigger adaptive immunity (DCs)

    8. Soluble innate recognition and complement activation

    9. Innate Immune Activation of Complement Pathway: 2 modes of initiation

    10. Recognition of an infection once it gets past the epithelial barrier Soluble innate immune recognition elements (collectins, ficolins, complement) Sentinel innate immune cells of tissues: tissue macrophages, mast cells and immature dendritic cells, which induce inflammation (all 3) and trigger adaptive immunity (DCs)

    11. Induction of Inflammation following recognition of pathogens

    12. Innate immune recognition of bacterial cell wall components

    13. NOD1 & NOD2 recognize peptidoglycan substructures and promote innate immune responses

    14. Toll-like receptors and recognition of pathogens

    15. Delivery of LPS to TLR4 by lipid transfer proteins

    16. Cellular location of TLRs

    17. Toll-like receptor signaling pathways

    18. Pathways of NF-kB activation

    19. Genes regulated by NF-kB

    20. Leukocyte recruitment to sites of inflammation

    21. Sepsis Syndrome Bacterial septicemia leads to activation of TLRs on monocytes in the blood Systemic release of TNF and IL-1 leads to “inflammation” all over the body Shock from loss of blood pressure (vasodilation and leakage of fluid into tissues) TLRs also induce coagulation (via tissue factor) The combination of effects can lead to multi-organ failure and death

    22. Inflammation Pro-inflammatory cytokines (TNF, IL-1) signal to endothelial cells to make them: Leaky to fluid (influx of plasma; containing antibodies, complement components, etc.) Sticky for leukocytes, leading to influx of neutrophils first, then monocytes, lymphocytes Systemic effects: fever, acute phase response Inflammation may also be triggered by complement activation or by activation of the coagulation system

    23. Inflammation: Neutrophils vs. Monocytes Acute inflammation is initially characterized as rich in neutrophils; later it is more monocytes. This is controlled by which chemokines are expressed by the endothelial cells. Neutrophils are dedicated to killing bacteria and are short-lived. They often damage host tissue as a byproduct.

    24. Inflammation: Neutrophils vs. Monocytes Acute inflammation is initially characterized as rich in neutrophils; later it is more monocytes. This is controlled by which chemokines are expressed by the endothelial cells. Neutrophils are dedicated to killing bacteria and are short-lived. They often damage host tissue as a byproduct. Monocytes are multi-potential, depending on cytokine signals: +IFN-g: assume a vigorous killing phenotype similar to neutrophils +IL-10: assume a wound-healing type phenotype (to clean up after infection is cleared) +GM-CSF: assume a dendritic cell phenotype and propagate adaptive immune priming

    25. Phagocytosis

    26. Opsonins and Phagocytic receptors

    27. Phagocytosis

    28. Phagocytosis and killing

    29. Phagocytosis and killing

    30. Viral Immunity Viruses evolve extremely rapidly, great challenge for innate immunity Anti-viral immunity has 2 roles Blocking infection (antibodies, complement, etc.) Blocking viral replication (interferon, killing infected cells) Viruses have evolved many mechanisms of evading immunity

    31. Anti-retroviral defense by a cytidine deaminase APOBEC3G

    32. Virus-infected cell produces interferon to act on neighboring cells

    33. Production of interferon by infected cells

    35. Anti-viral effects of interferon a/b

    36. Viral evasion of interferon: PKR

    39. NK cells can kill virus-infected cells (hypothesis: balance between activating and stimulating receptors)

    40. Recognition mechanisms of innate immunity (summary of examples)

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