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NUTRITION, INFECTION & THE IMMUNE SYSTEM. Ahmed A Wadee Immunology Division NHLS & School of Pathology University of the Witwatersrand (082 807 2628). Alimentary Tract. General defense mechanisms Mucous secretions Integrity of mucosal epithelium
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NUTRITION, INFECTION & THE IMMUNE SYSTEM Ahmed A Wadee Immunology Division NHLS & School of Pathology University of the Witwatersrand (082 807 2628)
AlimentaryTract • General defense mechanisms • Mucous secretions • Integrity of mucosal epithelium • Peristaltic motions of the gut propel contents downward • Secretory IgA and phagocytic cells • Stomach • Generally sterile due to low pH • Small Intestine • Upper portion contains few bacteria • As distal end of ilieum is reached flora increases • Colon • Enormous numbers of microorganisms • 50-60% of fecal dry weight is bacteria
Multiple Factors Protect Against GI Pathogens • Saliva • Stomach acid & enzymes • Bile • Water and electrolyte secretion • Mucosal products (mucus, defensins) • Epithelial barrier • Peristalsis • Bacterial flora
The Human Gut Flora • Rapidly colonises gut after birth • Comprises more than 1014 organisms • More than 400 species • Symbiotic relationship with host (commensals) • Weighs 1-2 kg
The Immune System of The Gut • The gut is the major site of contact in the body for foreign antigens • Gastrointestinal diseases kill more than 2 million people every year • Non-specific (innate) immunity • Specific immunity
Major components of the innate immune response • Cell mediated • Phagocytic cells • NK cells (natural killer) • Humoral • Complement • Acute phase proteins
Immune Cells and Innate Immunity • Phagocytes • Neutrophils • Monocyte/macrophage • Eosinophils (to a lesser extent) • NK cells (large granular lymphocytes) • Antibody-dependent cell-mediated cytotoxicity (ADCC) • Have two major functions • Lysis of target cells • Production of cytokines (IFN-γ and TNF-a) • Act against intracellular pathogens • Herpesviruses, Leishmania, Listeria monocytogenes • Act against protozoa • Toxoplasma, Trypanasoma
Organisation of the Mucosal Immune system (specific) • Gut Associated Lymphoid Tissue (GALT) / Mucosa Associated Lymphoid Tissue (MALT) • Tonsils • Adenoids • Peyer’s patches • Appendix • Intra-epithelial lymphocytes (IEL’s) • Lamina propria lymphocytes
Intra-epithelial Lymphocytes • Found between intestinal epithelial cells • CD8+ cells • Cytotoxic • Many are TcRgd+ • Produce IL2 ,IFNg & IL5 • Large granular lymphocytes
Lymphocytes in the Lamina Propria • Found in the epithelium & connective tissue of Lamina Propria • Mostly activated CD4+ (T helper cells) • TH1 cells: cell mediated responses (intracellular pathogens) • TH2 cells: antibody mediated responses (allergens, parasites, helminths) • Activated B cells; plasma cells IgA
Immunoglobulin A (IgA) • The major immunoglobin in the body-GUT • The GI tract is major source • Synthesised by plasma cells (B cells) in lamina propria • Transported via epithelium • Protects against infectious agents • Prevents attachment of bacteria or toxins to epithelia
Location of M Cells Found in: Peyer’s patches Intestinal epithelium Mucosa associated lymphoid aggregates (tonsils)
The Gut is Challenged by Foreign Antigens Regularly No Response (Tolerance) Response (Immune Activation) mucosal barrier
APC migrate to lymph nodes T cells activated in lymph nodes T cells migrate to tissue Inflammation/pathogen eradication Gut Immune Responses
Interaction of helper T cells (CD4+) and B cells in Lymphoid Tissues
MHC Class I or II restricted Antigen Presentation to T cells
Class II MHC – associated presentation of extra-cellular antigen to helper T cells + Class II MHC- associated antigen APC Extracellular Antigen CD4+ Helper T Lymphocyte cytokines
+ Intracellular Antigen Class I MHC- associated antigen APC CD8+ Cytotoxic T Lymphocyte Lysis of antigen-expressing target cell Class I MHC – associated presentation of intra-cellular antigen to cytotoxic T cells
CD4+ Helper T Lymphocytes secrete Distinct Sets of Cytokines TH1 cells produce IL2 and IFNg TH2 cells produce IL4, IL5, IL10 Which in turn determine the type of effector function (i.e. macrophage or CTL activation or B cell stimulation)
Local Immunity in the Small Intestine • Enterocytes secrete TGF-β, IL1, IL6 etc • Panath cells produce microbicidal proteins • Enterocytes promote migration and activity of lymphocyte populations in the villi
Nutrient Deficiencies & Immune Responses Malnutrition mainly affects: • Cell-mediated immunity • Phagocyte function • Complement activity • IgA production • Cytokine production • Lymphoid tissue - ‘nutritional thymectomy’
Malnutrition and Immunity Loss of fat cells results in low leptin (adipose tissue-derived hormone) levels: • signals nutritional status to the hypothalamus • modifies pro-inflammatory immune responses • provides a key link between nutritional deficiency and immune dysfunction
Protein-energy Malnutrition Associated with reduced • Numbers of CD4 helper T cells • CD4/CD8 ratios • Macrophage activation • Levels of C3,C5 and Factor B opsonisation phagocytosis • Intracellular killing of bacteria by phagocytes • Lysosyme levels • TNF &IL2 • Wound healing
Magnesium, Iron and Zinc Deficiency • Impairs CMI (TH1) & phagocyte function • Reduced CD4/CD8 ratios • Post-operative patients, athletes, elderly • Chronic deficiency seems to be associated with acute lymphoblastic leukemia and malignant lymphoma (Mg & Zn) • Altered NK and macrophage cytotoxicity (may affect tumor surveillance)
Vitamin Deficiency Vitamin A deficiency • Alters epithelial structure metaplasia & increased bacterial binding • Reduced T cell numbers and CMI Vitamin B6 and folate deficiencies • Reduced CMI • Reduced antibody production
Obesity and Immunity Obesity negatively affects:- • Cytotoxicity • NK cell function • Phagocyte function (bacteria & fungi) • Levels of micronutrients, lipids and hormones
Malnutrition & Infection Aggravate each other! Affect clinical outcomes of:- • Pneumonia • Diarrhoea • Measles • Tuberculosis HIV
HIV/AIDS • HIV/AIDS has a negative impact on nutritional status and may lead to malnutrition • Malnutrition weakens the immune system and increases vulnerability to opportunistic infections • Opportunistic infections cause symptoms such as anorexia and fever that reduce food intake and nutrient utilisation and increase nutrient requirements. • Reduced food intake and poor nutrient absorption weaken the immune system and hasten disease progression.
Oral Tolerance/Vaccination Effects are:- • Systemic (non-mucosal sites) • Dominant (transferable to naïve cells) • Produce local IgA and systemic IgG Ingested antigens may provide tolerance or protection
Applications • Polio vaccine • Protein antigens to induce tolerance to food proteins • Possible tolerance in autoimmunity • Mucosal adjuvants/vaccines, eg bacteria-viral combinations