the life history of t lymphocytes precursors mature in the thymus naïve cd4+ and cd8+ t cells enter...
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The life history of T lymphocytes
Precursors mature in the thymus
Naïve CD4+ and CD8+ T cells enter the circulation
Naïve T cells circulate through lymph nodes and find antigens
Clonal expansion; differentiation into effector and memory cells
Effector T cells migrate to sites of infection
Eradication of infection
Lecture outline
• Properties and functions of subsets of CD4+ effector T cells; functions of cytokines
• Activation and functions of CTLs
• Cell-mediated immunity: T cell-mediated defense against intracellular microbes
• Migration of T cells; activation of phagocytes and other leukocytes by effector T cells
Functions of CD4 helper T cells, the master controllers of immune responses, are mediated by
cytokines
Discovery of Th1 and Th2 subsets
• Immune responses to mycobacteria and helminths are very different but CD4+ T cells are required for both – How can the “same” CD4+ T cells
trigger such distinct reactions?
Discovery of Th1 and Th2 subsets
• Immune responses to mycobacteria and helminths are very different but CD4+ T cells are required for both – How can the “same” CD4+ T cells
trigger such distinct reactions?
• Hypothesis: CD4+ T cells consist of subpopulations that mediate different responses
• Identification of mouse CD4+ Th1, Th2 clones that produce distinct cytokines
The discovery of the Th17 subset
• The first two subsets were identified on the basis of distinct cytokine profiles and were called type 1 and type 2 helper cells (Th1 and Th2)
• Many inflammatory diseases (mouse models first) thought to be caused by Th1 cells were not prevented by eliminating Th1 cells or their cytokines
• Led to the discovery of the Th17 subset (annoying nomenclature!)
CD4+ TH subsets
Abbas, Lichtman and Pillai. Cellular and Molecular Immunology, 7th edition, 2011 c Elsevier
CD4+ T cell subsets: definitions and general properties
• Populations of CD4+ T cells that make restricted and non-overlapping sets of cytokines – Early after activation, T cells can
produce multiple cytokines– Progressive activation leads to
“polarization”: production of selected cytokines
• Distinct functions, migration properties, roles in disease
TH1 cells stimulate phagocyte-dependent host defense, the defense mechanism that works against most bacteria and viruses that enter tissues and are ingested by phagocytes
Effector functions of TH1 Cells
Development of TH1 cells
Th1 cells develop in response to microbes that activate dendritic cells and macrophages (most ingested bacteria and viruses).
Th2 cells combat helminths, provide defense at mucosal barriers (“barrier immunity”), and are involved in allergic reactions.
Effector functions of TH2 Cells
Antibody production
IgG4 (human), IgG1 (mouse)
Th2 cells develop in response to organisms that induce the local production of IL-4 and do not activate macrophages and dendritic cells strongly.
Development of TH2 cells
Th17 cells combat extracellular bacteria and fungi.These microbes activate DCs to produce Th17-inducing cytokines.
Th17 cells are also involved in many inflammatory diseases.
Effector functions of TH17 Cells
Inflammation
Chemokines, TNF, IL-1, CSF
s
Helper T cell subsets
• CD4+ helper T cells orchestrate specialized immune responses to different types of microbes
• The development of different Th subsets is driven by cytokines produced by APCs and other cells when naïve CD4 cells are being activated– Each subset is induced by the types of microbes
that subset is designed to combat
• Once a subset is generated, it makes cytokines that induce more of the same and shut off the others --> polarization of the immune response towards increasing specialization (a feature of adaptive immunity)
Genetic proof for the importance of different T cell subsets in humans
• Mutations affecting IL-12/IFN-g cytokines or receptors defective Th1 responses atypical mycobacterial infections
• Mutations affecting Th17 development or IL-17 mucocutaneous candidiasis and bacterial abscesses (“Job’s syndrome”)
16
Roles of T cell subsets in disease • Th1: autoimmune and inflammatory
diseases (IBD?, MS?, RA?); tissue damage in infections (e.g. Tb) – Activation of macrophages, CTL
responses; production of injurious antibodies
• Th2: allergies (e.g. asthma) – Stimulation of IgE responses, activation
of eosinophils
• Th17: inflammatory diseases (MS, IBD, RA, psoriasis)– Recruitment of leukocytes
(inflammation)
The balance of Th1 and Th2 responses determines the outcome of some infections
Cytotoxic (cytolytic) T lymphocytes (CTLs)
• CD8+ CD4- cells that recognize class I MHC-associated peptides derived from cytoplasmic protein antigens in any nucleated cell
• Effector functions:– Killing of infected cells (microbes in
cytoplasm), tumor cells (tumor antigens in cytoplasm)
– Secretion of IFN-g --> activation of macrophages (when microbes escape into cytoplasm and antigens enter class I MHC pathway)
CTLs “inject” their granule contents into target cells through membrane “pores”; major granule contents are enzymes that activate caspases and induce apoptotic death of the target cells, i.e. help the target cells to commit suicide
Mechanisms of killing of infected cells by CD8+ CTLs
In defense against intracellular microbes,T cells provide specificity and activate phagocytes, phagocytes kill the bacteria
Cell-mediated immunity against the intracellular bacterium Listeria monocytogenes
Cell-mediated immunity (CMI)
• Defense against intracellular microbes
• Mediated by T lymphocytes– CD4+ T cells activate phagocytes
(macrophages and neutrophils), eosinophils
– CD8+ T cells kill infected cells, activate macrophages
– T cell-mediated leukocyte recruitment and macrophage activation also cause delayed type hypersensitivity (DTH), which may have injurious effects
Stages in the development of T cell responses: induction
Stages in the development of T cell responses: effector phase
Naïve T cells migrate preferentially to secondary lymphoid organs, previously activated T cells to sites of infection and inflammation.Cell migration is regulated by adhesion molecules and chemokines.
Migration of naïve and effector T cells
T cells are retained at sites of antigen recognition in peripheral tissues, because antigen recognition stimulates expression of high-affinity adhesion receptors (integrins) that bind to extracellular matrix
Retention of effector T cells at sites of infection
Determinants of migration of naïve and effector T cells
• Naïve T cells: – L-selectin: binds to HEV in lymph nodes – CCR7: recognizes chemokines made in
peripheral lymphoid organs (lymph nodes, spleen, etc)
• Effector T cells: – Ligands for E- and P-selectins: bind to
endothelium at sites of infection– Various chemokine receptors: recognize
chemokines made at sites of infection– Increased expression of integrins: bind
to extracellular matrix proteins
Functions of CD4+ T cells are mediated by CD40-ligand and cytokines
Mutations of CD40L (or CD40) are the cause of a human disease associated with defects in antibody responses and CMI
Requirement for cell-cell contact ensures T cells recognize macrophages or B cells with the relevant antigen
Therapeutic applications:inhibit abnormal immuneresponses, graft rejection with anti-CD40L antibody
T cells (via CD40L, IFN) stimulate production of microbicidal substances in macrophages -- make phagocytes better able to kill what they eat.
Activation of macrophages by T cells
Functions of activated macrophages in CMI
Macrophage response Role in CMI
Production of reactive oxygenspecies, nitric oxide, lysosomal enzymes
Killing of microbes inphagolysosomes (maineffector function)
Secretion of cytokines (TNF, IL-1, chemokines, others)
Leukocyte recruitment(inflammation)
Increased expression of B7 costimulators, MHCmolecules
Increased T cellactivation (adaptiveimmunity)
Macrophages are activated by TLR recognition of microbes as part of innate immunity; T cells activate them more
Classical and alternative macrophage activation
The life history of T lymphocytes
Precursors mature in the thymus
Naïve CD4+ and CD8+ T cells enter the circulation
Naïve T cells circulate through lymph nodes and find antigens
Clonal expansion; differentiation into effector and memory cells
Effector T cells migrate to sites of infection
Eradication of infection