Tolerance, autoimmunity and the pathogenesis of immunemediated inflammatory diseases. Abul K. Abbas UCSF

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1 Tolerance, autoimmunity and the pathogenesis of immunemediated inflammatory diseases Abul K. Abbas UCSF

2 Balancing lymphocyte activation and control Activation Effector T cells Tolerance Regulatory T cells Normal: reactions against pathogens Inflammatory disease, e.g. reactions against self No response to self Controlled response to pathogens

3 The importance of immune regulation To avoid excessive lymphocyte activation and tissue damage during normal protective responses against infections To prevent inappropriate reactions against self antigens ( self-tolerance ) Failure of control mechanisms is the underlying cause of immune-mediated inflammatory diseases

4 General principles of controlling immune responses Responses against pathogens decline as the infection is eliminated Apoptosis of lymphocytes that lose their survival signals (antigen, etc) Memory cells are the survivors Active control mechanisms may function to limit responses to persistent antigens (self antigens, possibly tumors and some chronic infections) Often grouped under tolerance

5 Immunological tolerance Definition: specific unresponsiveness to an antigen that is induced by exposure of lymphocytes to that antigen (tolerogen vs immunogen) Significance: All individuals are tolerant of their own antigens (self-tolerance); breakdown of self-tolerance results in autoimmunity Therapeutic potential: Inducing tolerance may be exploited to prevent graft rejection, treat autoimmune and allergic diseases, and prevent immune responses in gene therapy

6 Autoimmunity Definition: immune response against self (auto-) antigen, by implication pathologic Disorders are often classified under immunemediated inflammatory diseases General principles: Pathogenesis: Susceptibility genes + environmental triggers Systemic or organ-specific

7 Central and peripheral tolerance The principal fate of lymphocytes that recognize self antigens in the generative organs is death (deletion), BUT: Some B cells may change their specificity (called receptor editing ) Some CD4 T cells may differentiate into regulatory (suppressive) T lymphocytes From Abbas, Lichtman and Pillai. Cellular and Molecular Immunology 6th ed, 2007

8 Consequences of self antigen recognition in thymus From: Abbas & Lichtman, Cellular & Molecular Immunology 5th ed 2003

9 Central tolerance Lymphocytes that see self antigens before they are mature are either eliminated or rendered harmless Probably continues to occur at some level throughout life (as new lymphocytes are produced from bone marrow stem cells) Role of the AIRE protein in thymic expression of some tissue antigens

10 Peripheral tolerance Normal T cell response APC CD28 TCR T cell Activated T cells Anergy APC TCR Off signals Functional unresponsiveness Deletion APC Activated T cell Apoptosis (activation-induced cell death) Suppression APC Block in activation Regulatory T cell

11 T cell anergy

12 T cell anergy Multiple mechanisms demonstrated in different experimental systems No clear evidence that natural self antigens induce T cell anergy (especially in humans) Therapeutic potential: can we administer antigens in ways that induce T-cell anergy?

13 Activation-induced cell death : death of mature T cells upon recognition of self antigens From Abbas and Lichtman. Basic Immunology 2nd ed, 2006 Both pathways cooperate to prevent reactions against self

14 Regulatory T cells From Abbas, Lichtman and Pillai. Cellular and Molecular Immunology 6th ed, 2007

15 Properties of regulatory T cells Phenotype: CD4, high IL-2 receptor (CD25), low IL-7 receptor, Foxp3 transcription factor; other markers Mechanisms of action: multiple secretion of immune-suppressive cytokines (TGFβ, IL-10, IL-35), inactivation of dendritic cells or responding lymphocytes

16 Thymic ( natural ) regulatory T cells (Treg) Development requires recognition of self antigen during T cell maturation Reside in peripheral tissues to prevent harmful reactions against self

17 Peripheral (adaptive, inducible) regulatory T cells Develop from mature CD4 T cells that are exposed to persistent antigen in the periphery; no role for thymus May be generated in all immune responses, to limit collateral damage Can be induced in vitro (stimulation of CD4 T-cells in presence of TGFβ + IL-2) What factors determine the balance of effector cells and Treg?

18 Signals for the generation and maintenance of regulatory T cells Antigen recognition, with or without inflammation? TGF-β (source?) Interleukin-2 (originally identified as T cell growth factor; major function is to control immune responses by maintaining functional Treg; works via Stat5) Low levels of B7: CD28 costimulation Transcription factor Foxp3 Many activated T cells (not only Treg) may transiently express Foxp3

19 Regulatory T cells Explosion of information about the generation, properties, functions and significance of these cells Some autoimmune diseases are associated with defective generation or function of Tregs or resistance of effector cells to suppression by Tregs Will cellular therapy with ex vivo expanded Treg become a reality? Therapeutic goal: selective induction or activation of Treg in immune diseases

20 Immune-mediated inflammatory diseases Chronic diseases with prominent inflammation, often caused by failure of tolerance or regulation RA, IBD, MS, psoriasis, many others Affect 2-5% of people, incidence increasing May result from immune responses against self antigens (autoimmunity) or microbial antigens (Crohn s disease?) May be caused by T cells and antibodies May be systemic or organ-specific

21 Features of autoimmune diseases Fundamental problem: imbalance between immune activation and control Underlying causative factors: susceptibility genes + environmental influences Immune response is inappropriately directed or controlled; effector mechanisms of injury are the same as in normal responses to microbes Nature of disease is determined by the type of dominant immune response Many immunological diseases are chronic and self-perpetuating

22 Pathogenesis of autoimmunity Susceptibility genes Failure of self-tolerance Persistence of functional self-reactive lymphocytes Environmental trigger (e.g. infections, tissue injury) Activation of self-reactive lymphocytes Immune responses against self tissues

23 Genetics of autoimmunity Human autoimmune diseases are complex polygenic traits Identified by genome-wide association mapping Single gene mutations are useful for pathway analysis Some polymorphisms are associated with multiple diseases May control general mechanisms of tolerance and immune regulation Other genetic associations are diseasespecific May influence end-organ damage

24 Genetics of autoimmunity: recent successes of genomics NOD2: polymorphism associated with ~25% of Crohn s disease Microbial sensor PTPN22: commonest autoimmunityassociated gene; polymorphism in RA, SLE, others Phosphatase CD25 (IL-2Rα): associated with MS, others; genome-wide association mapping Role in Tregs

25 Infections and autoimmunity Infections trigger autoimmune reactions Clinical prodromes, animal models Autoimmunity develops after infection is eradicated (i.e. the autoimmune disease is precipitated by infection but is not directly caused by the infection) Some autoimmune diseases are prevented by infections (type 1 diabetes, multiple sclerosis, others? -- increasing incidence in developed countries): mechanism unknown The hygiene hypothesis

26 Immune-mediated diseases The nature of the disease is determined by the type of dominant immune response Th1 response: inflammation, autoantibody production; autoimmune diseases Th2 response: IgE+eosinophil-mediated inflammation; allergic reactions Th17 response: acute (and chronic?) inflammation; increasingly recognized in immune-mediated diseases

27 Naïve CD4 T cell CD4 T cell subsets: function Th1 cells (IFN-γ) Host defense: many microbes Systemic and organ-specific autoimmune diseases Th2 cells (IL-4, IL-5) Host defense: helminths Allergic diseases Regulatory T cells Th17 cells (IL-17) Host defense: fungi, bacteria Organ-specific autoimmune diseases

28 Naïve CD4 T cell CD4 subsets: generation and function Th1 cells (IFN-γ) Host defense: many microbes Systemic and organ-specific autoimmune diseases Th2 cells (IL-4, IL-5) Host defense: helminths Allergic diseases Th17 cells (IL-17) TGF-β, IL-2: Foxp3, Stat5 Host defense: fungi, bacteria Organ-specific autoimmune diseases Regulatory T cells

29 Subsets of CD4+ T cells Dominant T cell subsets determine disease vs protection Many autoimmune and allergic diseases are associated with imbalance of T cell subsets Cytokines and transcription factors involved in differentiation of naïve T cells to different subsets are well defined, especially in vitro Conditions for induction in vivo? in disease? Stability or plasticity of subsets?

30 Immune-mediated diseases Immunological diseases tend to be chronic and self-perpetuating, because -- The initiating trigger can often not be eliminated (self antigen, commensal microbes) The immune system contains many built-in amplification mechanisms whose normal function is to optimize our ability to combat infections Epitope spreading

31 Amplification loop in cell-mediated immunity Cytokines are powerful amplifiers of immune reactions

32 Pathogenesis of organ-specific autoimmunity Current therapies target late stages of the reaction (lymphocyte activation, inflammation). Ultimate goal should be to tackle the underlying cause and restore control of the abnormally directed response

33 Immune-mediated inflammatory diseases Immune-mediated inflammatory diseases develop because the normal controls on immune responses fail The phenotype of the disease is determined by the nature of the immune response These diseases often become selfperpetuating

34 Animal models of human inflammatory diseases: how good are they? Resemblance to human diseases: Same target organs involved Often similar effector mechanisms (antibodies, cytokines, cytotoxic T lymphocytes) Differences from human diseases: Unknown underlying susceptibility genes (some similarities, e.g. in type 1 diabetes) Often induced by experimental manipulation, e.g. overt immunization with tissue antigen, inflammatory stimulus, or transgenic approach The potential of humanized mice?

35 Biomarkers of human immune diseases Major goal of current research High-throughput screens for transcripts and proteins associated with disease Many practical limitations: Reliance on population assays, even though only a small fraction of total lymphocytes may be abnormal in control/activation Use of blood cells, even though the relevant reactions may be in tissues Nevertheless, emerging successes: Type I interferon signature in lupus

36 Immune-mediated inflammatory diseases Experimental models are revealing pathways of immune regulation and why it fails Genetic studies are identifying underlying defects in human diseases Improving technologies are enabling analyses of patients Challenges: From genes to pathways (molecular and functional) Using the knowledge to develop therapies