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IMMUNOLOGY in SURGICAL PATIENT BY PROF. MOH. ALDAWBALY.ppt

Immunological reactions that happened in surgical patients

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IMMUNOLOGY By Dr Moh.S Aldawbali Ass.Prof of Surgery (SU) M.D M.R.C.S Mobile 771802020
Infection and Immunity Balance infection immunity Bolus of infection x virulence immunity Disease =
Definition of terms  Immunology  The study of immune system or immunity  the study of all aspects of host defense against infection and of adverse consequences of immune responses.  The study of the physiological mechanisms which enable the body to recognize materials as foreign and to neutralize, metabolize or eliminate them without injury to the host tissue.
 Immunity  State of protection from infectious diseases Immune system  A remarkably versatile defense system that has evolved to protect animals from invading pathogenic microorganisms and cancer.  It is able to generate an enormous variety of cells and molecules capable of specifically recognizing and eliminating an apparently limitless variety of foreign invaders. cont…
The immune system Immune System Innate (Nonspecific) Adaptive (Specific) Cellular Components Humoral Components Cell-Mediated Humoral (Ab)
Overview of the Immune System The immune system
The Innate immunity Natural immune system (Innate Immunity)  Non – specific  First line of defense  Repeated exposure - no augmentation  Components  Biochemical  Physical  Cells
1. Components a. Biochemical  enzymes, C’, etc.  secretions  pH b. Physical  skin  cilia c. Cells  Phagocytes, NK 2. Example a. Burn response Lysozymes Mucus Sebaceous glands Skin Cilia: trachea Acid in stomach Commensal organisms in gut & vagina Spermine in semen cont…
cont…
 Overall non-specific reaction of body to injury or invasion – starts immediately with infection or trauma  Reactants may initiate, expand, or sustain the response  Can be acute (short duration) or become chronic (prolonged duration)  Has 4 cardinal signs: heat, pain, redness, loss of function resulting from: cont…
 Increased blood and plasma flow to the area  Increased capillary permeability by retraction of endothelial cells  mediated by vaso active agents such as histamine and prostaglandins.  derived from injured cells and later from cells that infiltrate the area.  Migration of leucocytes, particularly Neutrophils and macrophages, from the capillaries to the site of injury is due to a process called chemotaxis. cont…
 Migration of white cells, especially early migration of neutraphils then macrophages to the area  Increased release of mediators such as histamine from damaged mast cells – furthering capillary dilation  Increased concentration of acute phase reactants that can amplify and/or control the response  Complement – a series of enzymes normally circulating in an inactive form may be activated resulting in lysis or enhanced phagocytosis of cells cont…
External Innate Defense Systems Prevent entrance:  Structural barriers – effective with most microorganisms  Skin - epidermis = layers of tightly packed epithelial cells. Outer layer is dead cells and keratin, waterproofing protein  Inner layer skin - dermis = blood vessels, hair follicles, sweat glands, and sebaceous glands that produce an oily secretion called sebum  Cilia and cough reflex – helps expel microbe containing mucous  Sneeze cont…
External Innate Defense Systems Mucus - conjunctivae, alimentary, respiratory, and urogenital tracts • saliva, tears, and mucous secretions wash away invaders and contain antibacterial or antiviral substances. • acidity (pH 5.6) of sweat, sebaceous glands, vagina (pH 5) and stomach (pH 1) – unfriendly to many microorganisms  enzymes present in the skin and stomach, tears Normal flora - out compete pathogens for attachment sites on the epithelial cell surface and for necessary nutrients. cont…
Internal Innate Defense System To prevent expansion of penetration  Recognize carbohydrates not normally present on cells such as mannose  May cause nonspecific activation of white cells  Phagocytosis – by neutraphils, eosinophils, basophils, or macrophages, mast cells, and dendritic cells  Clotting mechanism which entraps organisms in fibrin clots  Complement System can lyse cells or enhance phagocytosis cont…
Physiologic Barriers  Soluble factors contribute to innate immunity, they are collectively known as acute phase reactants.  Normal serum components, non-specific responders to inflammation  Increase because of infection, injury, trauma  Produced mostly by liver in response to inflammation and cytokine stimulation  Cytokines: IL-1, IL-6 and TNF alpha which are produced by macrophages and monocytes at inflammatory site are activators cont…
 Acute phase reactants are chemically varied and include:  C-reactive protein,  serum amyloid A,  mannose binding protein,  alpha-1 anti-trypsin,  haptoglobulin,  fibrinogen,  ceruloplasmin,  alpha-1 acid glycoprotein  Complement cont…
 Complement – a series of enzymes normally circulating in an inactive form  May be activated by the classical or alternate pathways  Can result in lysis or enhanced phagocytosis of cells  Lysozyme, a hydrolytic enzyme in mucous secretions and in tears, can cleave the peptidoglycan layer of bacterial cell wall.  Interferon, proteins produced by virus-infected cells. Has many functions including ability to bind to nearby cells and induce a generalized antiviral state. cont…
C-Reactive Protein  Normally trace levels in serum  Early acute inflammation indicator:  increases within 4-6 hrs of infection or trauma  100 to 1000 fold increase serum concentration  concentration drops rapidly in serum when stimulus removed  Enhances opsonization, agglutination, precipitation, and classical pathway complement activation – enhances removal of irritant cont…
Phagocytosis  Phagocytic cells Chemotaxins such as  Complement components  Coagulation cascade proteins  Bacterial and viral products  Attract phagocytic cells including:  Mast cell, lymphocyte, macrophage, neutrophil products  Physical contact between phagocytic cell and foreign object results in  Formation of phagosome  Formation of phagolysosome  Digestion  Release of debris cont…
 Phagocytosis  Is a form of endocytosis.  Important body defense mechanism is process in which specialized cells engulf and destroy foreign particles such as microorganisms or damaged cells.  Macrophages and segmented Neutrophiils are the most important phagocytic cells. cont…
 Can be divided in to several stages:  chemotaxis – attraction of leukocytes or other cells by chemicals  Movement of neutraphils is influenced by chemotaxins – chemical messangers  Complement, proteins from coagulation,  Products from bacteria and viruses,  Secretions from mast cells, lymphocytes, macrophages, and other neutraphils cont…
 Phagocytosis ...  Adherence – binding of organism to the surface of phagocytic cell.  Engulfment:- is the injestion of m/os and formation of phagosomes.  Digestion – after the foreign particle or m/os is ingested, cytoplasm lysosome fuse with phagosome The enzymes of lysosome then contribute to microbial killing and lysis. cont…
Phagocytosis ... cont… Source: Kuby immunology 2007, 5th ed
The adaptive immune system Immune System Innate (Nonspecific) Adaptive (Specific) Cellular Components Humoral Components Cell-Mediated Humoral (Ab)
The adaptive immune system
Adaptive Immunity  Specific  Second line of defense  Repeated exposure - augmented – memory  Faster response  More vigorous response  Longer lasting response  Anamnestic Components Classic Immune System  Cells (Cell mediated) =CMI  Soluble Factors (Humoral immunity) = HI The adaptive immune system
 Capable of recognizing and selectively eliminating specific foreign microorganisms and molecules(i.e., foreign antigens).  Unlike innate immune responses, adaptive immune responses are reactions to specific antigenic challenges  Different populations of lymphocytes and their products are the major actors together with accessory cells – Antigen presenting cells (APCs)  Cardinal features are :  Specificity  Diversity , Memory, The adaptive immune system
Cardinal Features of adaptive Immune Responses  Specificity –  specific for distinct antigen, and  for different structural components of a single complex protein, polysaccharide, or other macromolecules.  Portions of such antigens recognized by individual lymphocytes are called determinants or epitopes.  This fine specificity exists because individual lymphocyte express membrane receptors able to distinguish subtle (slight) differences in structure between distinct antigens. The adaptive immune system
 Diversity- total number of antigenic specificities of the lymphocytes in an individual, called the lymphocyte repertoire, is extremely large.  estimated mammalian immune system can discriminate 109 to 1011 distinct antigenic date ruminants.  This property of the lymphocyte repertoire is called diversity. It is the result of variability in the structures of antigen- binding sites of lymphocyte receptors for antigens. The adaptive immune system
 Memory- Exposure of the immune system to foreign antigen:  enhances its ability to respond again to that antigen.  Responses to second and subsequent exposure to the same antigen, called secondary immune responses, are usually more rapid and larger than the first or primary immune response. The adaptive immune system
 An effective immune response involves three major groups of cells: Cellular Immunity (T lymphocytes), Humoral Immunity (B cells), and Accessory cells (antigen- presenting cells).  The two major populations of lymphocytes—B lymphocytes (B cells) of Humoral immunity and T lymphocytes (T cells) of Cellular Immunity provide us with our specific adaptive immunity The adaptive immune system
 Specialization –the immune system responds in distinct and special ways to different microbes, maximizing the efficiency of antimicrobial defense mechanisms. Thus, humoral immunity and cell mediated immunity are elicited by different classes of microbes or by the same microbe at different stages of infection (extra cellular & intra cellular)  Self –limitation- All normal immune responses returning the immune system to its resting or basal state with time after antigen stimulations, process called homeostasis. The adaptive immune system
Innate Immunity Adaptive Immunity Comparison of Innate and Adaptive Immunity • No memory • No time lag • Not antigen specific • A lag period • Antigen specific • Development of memory Summary of innate and adaptive immunity
Thank you for Attention and Attendance

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IMMUNOLOGY in SURGICAL PATIENT BY PROF. MOH. ALDAWBALY.ppt

  • 1.
    IMMUNOLOGY By Dr Moh.S Aldawbali Ass.Profof Surgery (SU) M.D M.R.C.S Mobile 771802020
  • 2.
    Infection and ImmunityBalance infection immunity Bolus of infection x virulence immunity Disease =
  • 3.
    Definition of terms Immunology  The study of immune system or immunity  the study of all aspects of host defense against infection and of adverse consequences of immune responses.  The study of the physiological mechanisms which enable the body to recognize materials as foreign and to neutralize, metabolize or eliminate them without injury to the host tissue.
  • 4.
     Immunity  Stateof protection from infectious diseases Immune system  A remarkably versatile defense system that has evolved to protect animals from invading pathogenic microorganisms and cancer.  It is able to generate an enormous variety of cells and molecules capable of specifically recognizing and eliminating an apparently limitless variety of foreign invaders. cont…
  • 5.
    The immune system ImmuneSystem Innate (Nonspecific) Adaptive (Specific) Cellular Components Humoral Components Cell-Mediated Humoral (Ab)
  • 6.
    Overview of theImmune System The immune system
  • 7.
    The Innate immunity Naturalimmune system (Innate Immunity)  Non – specific  First line of defense  Repeated exposure - no augmentation  Components  Biochemical  Physical  Cells
  • 8.
    1. Components a. Biochemical enzymes, C’, etc.  secretions  pH b. Physical  skin  cilia c. Cells  Phagocytes, NK 2. Example a. Burn response Lysozymes Mucus Sebaceous glands Skin Cilia: trachea Acid in stomach Commensal organisms in gut & vagina Spermine in semen cont…
  • 9.
  • 10.
     Overall non-specificreaction of body to injury or invasion – starts immediately with infection or trauma  Reactants may initiate, expand, or sustain the response  Can be acute (short duration) or become chronic (prolonged duration)  Has 4 cardinal signs: heat, pain, redness, loss of function resulting from: cont…
  • 11.
     Increased bloodand plasma flow to the area  Increased capillary permeability by retraction of endothelial cells  mediated by vaso active agents such as histamine and prostaglandins.  derived from injured cells and later from cells that infiltrate the area.  Migration of leucocytes, particularly Neutrophils and macrophages, from the capillaries to the site of injury is due to a process called chemotaxis. cont…
  • 12.
     Migration ofwhite cells, especially early migration of neutraphils then macrophages to the area  Increased release of mediators such as histamine from damaged mast cells – furthering capillary dilation  Increased concentration of acute phase reactants that can amplify and/or control the response  Complement – a series of enzymes normally circulating in an inactive form may be activated resulting in lysis or enhanced phagocytosis of cells cont…
  • 13.
    External Innate DefenseSystems Prevent entrance:  Structural barriers – effective with most microorganisms  Skin - epidermis = layers of tightly packed epithelial cells. Outer layer is dead cells and keratin, waterproofing protein  Inner layer skin - dermis = blood vessels, hair follicles, sweat glands, and sebaceous glands that produce an oily secretion called sebum  Cilia and cough reflex – helps expel microbe containing mucous  Sneeze cont…
  • 14.
    External Innate DefenseSystems Mucus - conjunctivae, alimentary, respiratory, and urogenital tracts • saliva, tears, and mucous secretions wash away invaders and contain antibacterial or antiviral substances. • acidity (pH 5.6) of sweat, sebaceous glands, vagina (pH 5) and stomach (pH 1) – unfriendly to many microorganisms  enzymes present in the skin and stomach, tears Normal flora - out compete pathogens for attachment sites on the epithelial cell surface and for necessary nutrients. cont…
  • 15.
    Internal Innate DefenseSystem To prevent expansion of penetration  Recognize carbohydrates not normally present on cells such as mannose  May cause nonspecific activation of white cells  Phagocytosis – by neutraphils, eosinophils, basophils, or macrophages, mast cells, and dendritic cells  Clotting mechanism which entraps organisms in fibrin clots  Complement System can lyse cells or enhance phagocytosis cont…
  • 16.
    Physiologic Barriers  Solublefactors contribute to innate immunity, they are collectively known as acute phase reactants.  Normal serum components, non-specific responders to inflammation  Increase because of infection, injury, trauma  Produced mostly by liver in response to inflammation and cytokine stimulation  Cytokines: IL-1, IL-6 and TNF alpha which are produced by macrophages and monocytes at inflammatory site are activators cont…
  • 17.
     Acute phasereactants are chemically varied and include:  C-reactive protein,  serum amyloid A,  mannose binding protein,  alpha-1 anti-trypsin,  haptoglobulin,  fibrinogen,  ceruloplasmin,  alpha-1 acid glycoprotein  Complement cont…
  • 18.
     Complement –a series of enzymes normally circulating in an inactive form  May be activated by the classical or alternate pathways  Can result in lysis or enhanced phagocytosis of cells  Lysozyme, a hydrolytic enzyme in mucous secretions and in tears, can cleave the peptidoglycan layer of bacterial cell wall.  Interferon, proteins produced by virus-infected cells. Has many functions including ability to bind to nearby cells and induce a generalized antiviral state. cont…
  • 19.
    C-Reactive Protein  Normallytrace levels in serum  Early acute inflammation indicator:  increases within 4-6 hrs of infection or trauma  100 to 1000 fold increase serum concentration  concentration drops rapidly in serum when stimulus removed  Enhances opsonization, agglutination, precipitation, and classical pathway complement activation – enhances removal of irritant cont…
  • 20.
    Phagocytosis  Phagocytic cellsChemotaxins such as  Complement components  Coagulation cascade proteins  Bacterial and viral products  Attract phagocytic cells including:  Mast cell, lymphocyte, macrophage, neutrophil products  Physical contact between phagocytic cell and foreign object results in  Formation of phagosome  Formation of phagolysosome  Digestion  Release of debris cont…
  • 21.
     Phagocytosis  Isa form of endocytosis.  Important body defense mechanism is process in which specialized cells engulf and destroy foreign particles such as microorganisms or damaged cells.  Macrophages and segmented Neutrophiils are the most important phagocytic cells. cont…
  • 22.
     Can bedivided in to several stages:  chemotaxis – attraction of leukocytes or other cells by chemicals  Movement of neutraphils is influenced by chemotaxins – chemical messangers  Complement, proteins from coagulation,  Products from bacteria and viruses,  Secretions from mast cells, lymphocytes, macrophages, and other neutraphils cont…
  • 23.
     Phagocytosis ... Adherence – binding of organism to the surface of phagocytic cell.  Engulfment:- is the injestion of m/os and formation of phagosomes.  Digestion – after the foreign particle or m/os is ingested, cytoplasm lysosome fuse with phagosome The enzymes of lysosome then contribute to microbial killing and lysis. cont…
  • 24.
  • 25.
    The adaptive immunesystem Immune System Innate (Nonspecific) Adaptive (Specific) Cellular Components Humoral Components Cell-Mediated Humoral (Ab)
  • 26.
  • 27.
    Adaptive Immunity  Specific Second line of defense  Repeated exposure - augmented – memory  Faster response  More vigorous response  Longer lasting response  Anamnestic Components Classic Immune System  Cells (Cell mediated) =CMI  Soluble Factors (Humoral immunity) = HI The adaptive immune system
  • 28.
     Capable ofrecognizing and selectively eliminating specific foreign microorganisms and molecules(i.e., foreign antigens).  Unlike innate immune responses, adaptive immune responses are reactions to specific antigenic challenges  Different populations of lymphocytes and their products are the major actors together with accessory cells – Antigen presenting cells (APCs)  Cardinal features are :  Specificity  Diversity , Memory, The adaptive immune system
  • 29.
    Cardinal Features ofadaptive Immune Responses  Specificity –  specific for distinct antigen, and  for different structural components of a single complex protein, polysaccharide, or other macromolecules.  Portions of such antigens recognized by individual lymphocytes are called determinants or epitopes.  This fine specificity exists because individual lymphocyte express membrane receptors able to distinguish subtle (slight) differences in structure between distinct antigens. The adaptive immune system
  • 30.
     Diversity- totalnumber of antigenic specificities of the lymphocytes in an individual, called the lymphocyte repertoire, is extremely large.  estimated mammalian immune system can discriminate 109 to 1011 distinct antigenic date ruminants.  This property of the lymphocyte repertoire is called diversity. It is the result of variability in the structures of antigen- binding sites of lymphocyte receptors for antigens. The adaptive immune system
  • 31.
     Memory- Exposureof the immune system to foreign antigen:  enhances its ability to respond again to that antigen.  Responses to second and subsequent exposure to the same antigen, called secondary immune responses, are usually more rapid and larger than the first or primary immune response. The adaptive immune system
  • 32.
     An effectiveimmune response involves three major groups of cells: Cellular Immunity (T lymphocytes), Humoral Immunity (B cells), and Accessory cells (antigen- presenting cells).  The two major populations of lymphocytes—B lymphocytes (B cells) of Humoral immunity and T lymphocytes (T cells) of Cellular Immunity provide us with our specific adaptive immunity The adaptive immune system
  • 33.
     Specialization –theimmune system responds in distinct and special ways to different microbes, maximizing the efficiency of antimicrobial defense mechanisms. Thus, humoral immunity and cell mediated immunity are elicited by different classes of microbes or by the same microbe at different stages of infection (extra cellular & intra cellular)  Self –limitation- All normal immune responses returning the immune system to its resting or basal state with time after antigen stimulations, process called homeostasis. The adaptive immune system
  • 34.
    Innate Immunity AdaptiveImmunity Comparison of Innate and Adaptive Immunity • No memory • No time lag • Not antigen specific • A lag period • Antigen specific • Development of memory Summary of innate and adaptive immunity
  • 35.

Editor's Notes

  • #8 When a person is burned they lose skin and fluids. This results in multiple complications including high risk for infections.