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Immune Response – Anatomy, Structure, Functions

The Immune response is the body’s ability to stay safe by affording protection against harmful agents and involves lines of defense against most microbes as well as a specialized and highly specific response to a particular offender. This immune response classifies as either innate which is non-specific and adaptive acquired which is highly specific. The innate response, often our first line of defense against anything foreign, defends the body against a pathogen in a similar fashion at all times. These natural mechanisms include the skin barrier, saliva, tears, various cytokines, complement proteins, lysozyme, bacterial flora, and numerous cells including neutrophils, basophils, eosinophils, monocytes, macrophages, reticuloendothelial system, natural killer cells (NK cells), epithelial cells, endothelial cells, red blood cells, and platelets.

The adaptive acquired immune response will utilize the ability of specific lymphocytes and their products (immunoglobulins, and cytokines) to generate a response against the invading microbes and its typical features are[rx][rx][rx]:

Specificity – as the triggering mechanism is a particular pathogen, immunogen or antigen.
Heterogeneity – signifies the production of millions of different effectors of the immune response (antibodies) against millions of intruders.
Memory – The immune system has the ability not only to recognize the pathogen on its second contact but to generate a faster and stronger response.

The inflammatory immune response is an example of innate immunity as it blocks the entry of invading pathogens through the skin, respiratory or gastrointestinal tract. If pathogens can breach the epithelial surfaces, they encounter macrophages in the subepithelial tissues that will not only attempt to engulf them but also produce cytokines to amplify the inflammatory response.

Active immunity results from the immune system’s response to an antigen and therefore is acquired. Immunity resulting from the transfer of immune cells or antibodies from an immunized individual is passive immunity.

The immune system has evolved for the maintenance of homeostasis, as it can discriminate between foreign antigens and self; however, when this specificity is affected an autoimmune reaction or disease develops.

Issues of Concern

While the immune system is meant to protect the individual against threats, at times an exaggerated immune response generates a reaction against self-antigens leading to autoimmunity. Also, the immune system is not able to defend against all threats at all times.

Transplantation rejections are immune-mediated responses, represent a hindrance to transplantation
The etiology of many autoimmune disorders is obscure – the reality is that the prevalence of these disorders increases and manifests more aggressively
Type-I hypersensitivity disorders are immune-mediated and include allergic bronchial asthma, food allergy, and anaphylactic shock
Immunodeficiency disorders are rare, but they affect some children

Vaccination is required to induce an adequate active immune response to specific pathogens

Live attenuated vaccines: Induce both humoral and cellular response. Contraindicated in pregnancy and immunocompromised states. Examples include adenovirus, Polio (Sabin), Varicella, Smallpox, BCG, Yellow fever, Influenza (intranasal), MMR, Rotavirus, etc
Killed or inactivated vaccines: Induce only humoral response. Examples include rabies, influenza (injection), Polio (Salk), Hepatitis A, etc
Subunit vaccines: Examples include HBV, HPV (types 6,11,16 and 18), acellular pertussis, Neisseria meningitides, Streptococcus pneumoniae, Hemophilus influenza type b, etc
Toxoid vaccine: Examples include Clostridium tetani, Corynebacterium diphtheria, etc.

Cellular

Cells of the innate immunity are:

Phagocytes (monocytes, macrophages, neutrophils, and dendritic cells)
Natural killer (NK) cells

Cells of the adaptive response are:

T Lymphocytes classified as CD4+T cells and CD8+T cells
B Lymphocytes differentiate into plasma cells, which produce specific antibodies

Organ Systems Involved

The organ systems involved in the immune response are primarily lymphoid organs which include, spleen, thymus, bone marrow, lymph nodes, tonsils, and liver. The lymphoid organ system classifies according to the following:

Primary lymphoid organs (thymus and bone marrow), where T and B cells first express antigen receptors and become mature functionally.
Secondary lymphoid organs like the spleen, tonsils, lymph nodes, the cutaneous and mucosal immune system; this is where B and T lymphocytes recognize foreign antigens and develop appropriate immune responses.

T lymphocytes mature in the thymus, where these cells reach a stage of functional competence while B lymphocytes mature in the bone marrow the site of generation of all circulating blood cells. Excessive release of cytokines stimulated by these organisms can cause tissue damage, such as endotoxin shock syndrome.

Function

The immune system responds variedly to different microorganisms often determined by the features of the microorganism. These are some different ways in which the immune system acts

Immune Response to Bacteria

The response often depends on the pathogenicity of the bacteria[rx]:

Neutralizing antibodies are synthesized if the bacterial pathogenicity is due to a toxin
Opsonizing antibodies – produced as they are essential in destroying extracellular bacteria
The complement system is activated especially by gram-negative bacterial lipid layers
Phagocytes kill most bacteria utilizing positive chemotaxis, attachment, uptake and finally engulfing the bacteria
CD8+ T cells can kill cells infected by bacteria

Immune Response to Fungi [rx]

The innate immunity to fungi includes defensins and phagocytes
CD4+ T helper cells are responsible for the adaptive immune response against fungi
Dendritic cells secrete IL-12 after ingesting fungi, and IL-12 activates the synthesis of gamma interferon which activates the cell-mediated immunity

Immune Response to Viruses [rx]

Interferon, NK cells, and phagocytes prevent the spread of viruses in the early stage
Specific antibodies and complement proteins participate in viral neutralization and can limit spread and reinfection
Adaptive immunity is of foremost importance in the protection against viruses – these include CD8+ T cells that kill them and CD4+ T cells as the dominant effector cell population in response to many virus infections

Immune response to parasites[rx]

Parasitic infection stimulates various mechanisms of immunity due to their complex life cycle
Both CD4+ and CD8+ Cells protect against parasites
Macrophages, eosinophils, neutrophils, and platelets can kill protozoa and worms by releasing reactive oxygen radicals and nitric oxide
Increased eosinophil number and the stimulation of IgE by Th-2 CD4+ T cells are necessary for the killing of intestinal worms
Inflammatory responses also combat parasitic infections

Despite Immune response(s) generated by intact and functional Immune systems we still fall sick, and this is often due to evasive mechanisms employed by these microbes. Here are some of those.

Strategies of Viruses to Evade the Immune System

Antigenic variation: It is a mutation in proteins that are typically recognized by antibodies and lymphocytes. HIV continually mutates, thus making it difficult for either the immune system to protect against it and also hinders the development of a vaccine. By disrupting 2′,5′-oligoadenylate synthetase activity or by the production of soluble interferon receptors viruses disrupt the Interferon response.

By several mechanisms, Viruses affects the expression of MHC molecules.

A virus can infect immune cells: Normal T and B cells are also sites of virus persistence. HIV hides in CD4+T cells and EBV in B cells.

Strategies of Bacteria to Evade the Immune System

Intracellular pathogens may hide in cells: Bacteria can live inside metabolically damaged host leukocytes, and escaping from phagolysosomes (Shigella spp).

Other mechanisms:

Production of toxins that inhibit the phagocytosis
They are preventing killing by encapsulation
The release of catalase inactivates hydrogen peroxide
They infect cells and then cause impaired antigenic presentation
The organism may kill the phagocyte by apoptosis or necrosis

Strategies of Fungi to Evade the Immune System

Fungi produce a polysaccharide capsule, which inhibits the process of phagocytosis and overcoming opsonization, complement, and antibodies
Some fungi inhibit the activities of host T cells from delaying cell-mediated killing
Other organisms (e.g., Histoplasma capsulatum) evade macrophage killing by entering the cells via CR3 and their escape from phagosome formation

Strategies of Parasites to Evade the Immune System

Parasites can resist destruction by complement
Intracellular parasites can avoid being killed by lysosomal enzymes and oxygen metabolites
Parasites disguise themselves as a protection mechanism
Antigenic variation (e.g., African trypanosome) is an essential mechanism to evade the immune system
Parasites release molecules that interfere with the immune system normal function

Mechanism

The most important mechanisms of the immune system by which it generates immune response include:

Macrophages produce lysosomal enzymes and reactive oxygen species to eliminate the ingested pathogens. These cells produce cytokines that attract other leukocytes to the site of infection to protect the body. The innate response to viruses includes the synthesis and release of interferons and activation of natural killer cells that recognize and destroys the virus-infected cells. The innate immunity against bacterial consist of the activation of neutrophils that ingest pathogens and the movement of monocytes to the inflamed tissue where it becomes in macrophages. They can engulf, and process the antigen and then present it to a group of specialized cells of the acquired immune response. Eosinophils protect against parasitic infections by releasing the content of their granules.[rx][rx]

Antibody-dependent cell-mediated cytotoxicity (ADCC): A cytotoxic reaction in which Fc-receptor expressing killer cells recognize target cells via specific antibodies.
Affinity maturation: The increase in average antibody affinity mostly seen during a secondary immune response.
Complement system: It is a molecular cascade of serum proteins involved in the control of inflammation, lytic attack on cell membranes, and activation of phagocytes. The system can undergo activation by interaction with IgG or IgM (classical pathway) or by involving factors B, D, H, P, I, and C3, which interact closely with an activator surface to generate an alternative pathway C3 convertase.
Energy: It is the failure to induce an immune response following stimulation with a potential immunogen.
Antigen processing: Conversion of an antigen into a form that can be recognized by lymphocytes. It is the initial stimulus for the generation of an immune response.
Antigen presentation: It is a process in which specific cells of the immune system express antigenic peptides in their cell membrane along with alleles of the major histocompatibility complex (MHC) which is recognizable by lymphocytes.
Apoptosis: Programmed cell death involving nuclear fragmentation and the formation of apoptotic bodies.
Chemotaxis: Migration of cells in response to concentration gradients of chemotactic factors.
Hypersensitivity reaction: A robust immune response that causes tissue damage more considerable than the one caused by an antigen or pathogen that induced the response. For instance, allergic bronchial asthma and systemic lupus erythematosus are an example of type I and type III hypersensitivity reactions respectively.
Inflammation: Certain reactions that attract cells and molecules of the immune system to the site of infection or damage. It featured increased blood supply, vascular permeability and increased transendothelial migration of blood cells (leukocytes).
Opsonization: A process of facilitated phagocytosis by deposition of opsonins (IgG and C3b) on the antigen.
Phagocytosis: The process by which cells (e.g., macrophages and dendritic cells) take up or engulf an antigenic material or microbe and enclose it within a phagosome in the cytoplasm.
Immunological tolerance: A state of specific immunological unresponsiveness.

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Hypersensitivity Reactions

They are overreactive immune responses to antigens that would not normally cause an immune reaction.

Type 1 hypersensitivity reactions: Initial exposure to the antigen causes stimulates Th2 cells. They release IL-4 leading the B cells to switch their production of IgM to IgE antibodies which are antigen-specific. The IgE antibodies bind to mast cells and basophils, sensitizing them to the antigen.

When the body is exposed to the allergen again, it cross-links the IgE bound to the sensitized mast cells and basophils, causing the degranulation and release of preformed mediators including histamine, leukotrienes, and prostaglandins. This causes systemic vasodilation, bronchoconstriction, and increased permeability of vascular endothelium.

The reaction can be divided into two stages –

1) Immediate, in which release of preformed mediators cause the immune response, and
2) Late-phase response 8-12 hours later, in which the cytokines released in the immediate stage stimulate basophils, eosinophils, and neutrophils even though the allergen is removed.

Type 2 hypersensitivity reactions (Antibody dependant cytotoxic hypersensitivity): Immune response against the antigens present on the cell surface. Antibodies binding to the cell surface, activate the complement system and cause the degranulation of neutrophils and destruction of the cell. Such reactions can be targeted at self or non-self antigens. ABO blood group incompatibility leading to acute hemolytic transfusion reactions is an example of Type 2 hypersensitivity.

Type 3 hypersensitivity reactions – are also mediated by circulating antigen-antibody complex that may be deposited in and damage tissues. Antigens in type 3 relations are soluble as opposed to cell-bound antigens in type 2.

Type 4 hypersensitivity reactions (delayed-type hypersensitivity reactions): They are mediated by antigen-specific activated T-cells. When the antigen enters the body, it is processed by antigen-presenting cells and presented together with the MHC II to a Th1 cell. If the T-helper cell has already been sensitized to that particular antigen, it will be stimulated to release chemokines to recruit macrophages and cytokines such as interferon-γ to activate them. This causes local tissue damage. The reaction takes longer than all other types, around 24 to 72 hours.

Transplant Rejection

Xenografts are grafts between members of different species, trigger the maximal immune response. Rapid rejection.
Allografts are grafts between members of the same species.
Autografts are grafts from one part of the body to another. No rejection.
Isografts are grafts between genetically identical individuals. No rejection.

Hyperacute Rejection: In hyperacute rejection, the transplanted tissue is rejected within minutes to hours because vascularization is rapidly destroyed. Hyperacute rejection is antibody-mediated and occurs because the recipient has preexisting antibodies against the graft, which can be due to prior blood transfusions, multiple pregnancies, prior transplantation, or xenografts. Activation of the complement system leads to thrombosis in the vessels preventing the vascularization of the graft.

Acute Rejection: Develops within weeks to months. Involves the activation of T lymphocytes against donor MHCs. May also involve humoral immune response, which antibodies developing after transplant. It manifests as vasculitis of graft vessels with dense interstitial lymphocytic infiltrate.

Chronic Rejection: Chronic rejection develops months to years after acute rejection episodes have subsided. Chronic rejections are both antibody- and cell-mediated. The use of immunosuppressive drugs and tissue-typing methods has increased the survival of allografts in the first year, but chronic rejection is not prevented in most cases. It generally presents as fibrosis and scarring. In heart transplants, chronic rejection manifests as accelerated atherosclerosis. In transplanted lungs, it manifests as bronchiolitis obliterans. In liver transplants, it manifests as vanishing bile duct syndrome. In kidney recipients, it manifests as fibrosis and glomerulopathy.

Graft-versus-host Disease: The onset of the disorder varies. Grafted immunocompetent T cells proliferate in the immunocompromised host and reject host cells which they consider ‘nonself’ leading to severe organ dysfunction. It is a type 4 hypersensitivity reaction and manifests as maculopapular rash, jaundice, diarrhea, hepatosplenomegaly. Usually occurs in the bone marrow and liver transplants, which are rich in lymphocytes.

Related Testing

The immunological investigations for the study of innate and adaptive immunity are listed below and include the assessment of immunoglobulins, B and T-lymphocyte counts, lymphocyte stimulation assays, quantification of components of the complement system and phagocytic activity.[rx][rx][rx][rx][rx]

Quantitative Serum Immunoglobulins

IgG Sub-Classes

IgG1
IgG2
IgG3
IgG4

Antibody Activity

IgG antibodies (post-immunization)

Tetanus toxoid
Diphtheria toxoid
Pneumococcal polysaccharide
Polio

IgG antibodies (post-exposure)

Rubella
Measles
Varicella Zoster

Detection of isohemagglutinins (IgM)

Anti-type A blood
Anti-type B blood

Other assays

Test for heterophile antibody
Anti-streptolysin O titer
Immunodiagnosis of infectious diseases (HIV, hepatitis B, and C, HTLV and dengue)
Serum protein electrophoresis

Blood Lymphocyte Subpopulations

Total lymphocyte count
T lymphocytes (CD3, CD4, and CD8)
B lymphocytes (CD19 and CD20)
CD4/CD8 ratio

Lymphocyte Stimulation Assays

Phorbol ester and ionophore
Phytohemagglutinin
Antiserum to CD3

Phagocytic Function

Nitroblue tetrazolium (NBT) test (before and after stimulation with endotoxin)

Unstimulated
Stimulated

Neutrophil mobility

In medium alone
In the presence of chemoattractant

Complement System Evaluation

Measurement of individuals components by immunoprecipitation tests, ELISA, or Western blotting

C3 serum levels
C4 serum levels
Factor B serum levels
C1 inhibitor serum levels

Hemolytic assays

CH50
CH100
AH50

Complement system functional studies

Classical pathway assay (using IgM on a microtiter plate)
Alternative pathway assay (using LPS on a microtiter plate)
Mannose pathway assay (using mannose on a microtiter plate)

Measurement of complement-activating agents

Circulating immune complexes
Cold agglutinins

Assays for complement-binding

C1q autoantibody ELISA
C1 inhibitor autoantibody ELISA

Others complement assays

LPS activation assay
Specific properdin test
C1 inhibitor activity test

Autoimmunity Studies

Anti-nuclear antibodies (ANA)
Detection of specific auto-immune antibodies for systemic disorders (anti-ds DNA, rheumatoid factor, anti-histones, anti-Smith, anti-(SS-A) and anti-(SS-B)
Detection of anti-RBC, antiplatelet, and anti-neutrophil
Testing for organ-specific auto-immune antibodies

Microbiological Studies

Blood (bacterial culture, HIV by PCR, HTLV testing)
Urine (testing for cytomegalovirus, sepsis, and proteinuria)
Nasopharyngeal swab (testing for Rhinovirus)
Stool (testing for viral, bacterial or parasitic infection)
Sputum (bacterial culture and pneumocystis PCR)
Cerebrospinal fluid (culture, chemistry, and histopathology)

Coagulation Tests

Factor V assay
Fibrinogen level
Prothrombin time
Thrombin time
Bleeding time

Other Investigations

Complete blood cell count
Tuberculin test
Bone marrow biopsy
Histopathological studies
Liver function test
Blood chemistry
Tumoral markers
Serum levels of cytokines
Chest x-ray
Diagnostic ultrasound
CT scan
Fluorescent in situ hybridization (FISH)
DNA testing (for most congenital disorders)

Pathophysiology

The immune system protects the body against many diseases including recurrent infections, allergy, tumor, and autoimmunity. The consequences of an altered immunity will manifest in the development of many immunological disorders some of which are listed below:

X- linked agammaglobulinemia (Bruton disease)
Selective IgA Deficiency
Selective IgG deficiency
Congenital thymic aplasia (DiGeorge Syndrome)
Chronic mucocutaneous candidiasis
Hyper-IgM syndrome
Interleukin-12 receptor deficiency
Severe combined immunodeficiency disease (SCID)
ZAP-70 deficiency
Janus kinase 3 deficiency
RAG1 and RAG2 deficiency
Wiskott-Aldrich syndrome
Immunodeficiency with ataxia-telangiectasia
MHC deficiency (bare leukocyte syndrome)
Complement system deficiencies
Hereditary angioedema
Chronic granulomatous disease (CGD)
Leukocyte adhesion deficiency syndrome
Job syndrome
Chediak Higashi syndrome
Acquired immunodeficiency syndrome
Anaphylaxis
Allergic bronchial asthma
Allergic rhinitis
Allergic conjunctivitis
Food allergy
Atopic eczema
Drug allergy
Immune thrombocytopenia
Autoimmune hemolytic anemia
Autoimmune neutropenia
Systemic lupus erythematosus
Rheumatoid arthritis
Autoimmune hepatitis
Hemolytic disease of the fetus and the newborn (erythroblastosis fetalis)
Myasthenia gravis
Goodpasture syndrome
Pemphigus
Tuberculosis
Contact dermatitis
Leprosy
Insulin-dependent diabetes mellitus
Schistosomiasis
Sarcoidosis
Crohn disease
Autoimmune lymphoproliferative syndrome
X-linked lymphoproliferative disorder
Common variable immunodeficiency
B-cell chronic lymphocytic leukemia
B-cell prolymphocytic leukemia
Non-Hodgkin lymphoma (including mantle cell lymphoma) in leukemic phase
Hairy cell leukemia
Multiple myeloma
Splenic lymphoma with villous lymphocytes
Sezary syndrome
T-cell prolymphocytic leukemia
Adult T-cell leukemia-lymphoma
Large granulated lymphocyte leukemia
Leukocyte adhesion deficiency syndrome
Chronic active hepatitis
Coccidioidomycosis
Behcet disease
Aphthous stomatitis
Familial keratoacanthoma
Autoimmune polyendocrinopathy candidiasis ectodermal dystrophy
Idiopathic CD4+ lymphocytopenia
Complement system deficiencies
ADA-SCID
Artemis SCID
Newly diagnosed non-germinal center B-cell subtype of diffuse large B-cell lymphoma
Melanoma
Chagas disease

Functions

The immune system is organized into discrete compartments to provide the milieu for the development and maintenance of effective immunity. Those two overlapping compartments: the lymphoid and reticuloendothelial systems (RES) house the principal immunologic cells, the leukocytes. Leukocytes derived from pluripotent stem cells in the bone marrow during postnatal life include neutrophils, eosinophils, basophils, monocytes and macrophages, natural killer (NK) cells, and T and B lymphocytes. Hematopoietic and lymphoid precursor cells are derived from pluripotent stem cells. Cells that are specifically committed to each type of leukocyte (colony-forming units) are consequently produced with the assistance of special stimulating factors (e.g. cytokines).

Cells of the immune system intercommunicate by ligand-receptor interactions between cells and/or via secreted molecules called cytokines. Cytokines produced by lymphocytes are termed lymphokines (i.e., interleukins and interferon-γ) and those produced by monocytes and macrophages are termed monokines.

Lymphoid System

Cells of the lymphoid system provide highly specific protection against foreign agents and also orchestrate the functions of other parts of the immune system by producing immunoregulatory cytokines. The lymphoid system is divided into 1) central lymphoid organs, the thymus and bone marrow, and 2) peripheral lymphoid organs, lymph nodes, the spleen, and mucosal and submucosal tissues of the alimentary and respiratory tracts. The thymus instructs certain lymphocytes to differentiate into thymus-dependent (T) lymphocytes and selects most of them to die in the thymus (negative selection) and others to exit into the circulation (positive selection). T lymphocytes circulate through the blood, regulate antibody and cellular immunity, and help defend against many types of infections. The other classes of lymphocytes, B cells (antibody-forming cells) and natural killer (NK) cells are thymic-independent and remain principally in peripheral lymphoid organs.

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Reticuloendothelial System

Cells of the RES provide natural immunity against microorganisms by

1) a coupled process of phagocytosis and intracellular killing,
2) recruiting other inflammatory cells through the production of cytokines, and
3) presenting peptide antigens to lymphocytes for the production of antigen-specific immunity.

The RES consists of 1) circulating monocytes; 2) resident macrophages in the liver, spleen, lymph nodes, thymus, submucosal tissues of the respiratory and alimentary tracts, bone marrow, and connective tissues; and 3) macrophage-like cells including dendritic cells in lymph nodes, Langerhans cells in the skin, and glial cells in the central nervous system.

Leukocytes

Leukocytes, the main cells in the immune system, provide either innate or specific adaptive immunity. These cells are derived from myeloid or lymphoid lineage. Myeloid cells include highly phagocytic, motile neutrophils, monocytes, and macrophages that provide the first line of defense against most pathogens. The other myeloid cells, including eosinophils, basophils, and their tissue counterparts, mast cells, are involved in defense against parasites and in the genesis of allergic reactions. In contrast, lymphocytes regulate the action of other leukocytes and generate specific immune responses that prevent chronic or recurrent infections.

Myeloid Cells

Neutrophils: These are one of the major types of cells that are recruited to ingest, kill, and digest pathogens. Neutrophils are the most highly adherent, motile, phagocytic leukocytes and are the first cells recruited to acute inflammatory sites. Each of their functions is dependent upon special proteins, such as the adherence molecule CD11b/CD18, or biochemical pathways, such as the respiratory burst associated with cytochrome b₅₅₈.

Eosinophils: Eosinophils defend against many types of parasites and participate in common hypersensitivity reactions via cytotoxicity. That cytotoxicity is mediated by large cytoplasmic granules, which contain the eosinophilic basic and cationic proteins.

Basophils: These cells and their tissue counterparts, mast cells, produce cytokines that help defend against parasites and engender allergic inflammation. These cells display high-affinity surface membrane receptors for IgE antibodies and have many large cytoplasmic granules, which contain heparin and histamine. When cell-bound IgE antibodies are cross-linked by antigens, the cells degranulate and produce low-molecular-weight vasoactive mediators (e.g. histamine) through which they exert their biological effects.

Monocytes/Macrophages: Monocytes and macrophages are involved in phagocytosis and intracellular killing of microorganisms. Macrophages process protein antigens and present peptides to T cells. These monocytes/macrophages are highly adherent, motile, and phagocytic; they marshal and regulate other cells of the immune system, such as T lymphocytes; serve as antigen processing-presenting cells, and act as cytotoxic cells when armed with specific IgG antibodies.

Macrophages are differentiated monocytes, which are one of the principal cells found to reside for long periods in the RES. Macrophages may also be recruited to inflammatory sites, and be further activated by exposure to certain cytokines to become more effective in their biologic functions.

Lymphoid Cells

These cells provide efficient, specific, and long-lasting immunity against microbes and are responsible for acquired immunity. Lymphocytes differentiate into three separate lines: thymic-dependent cells or T lymphocytes that operate in cellular and humoral immunity, B lymphocytes that differentiate into plasma cells to secrete antibodies, and natural killer (NK) cells. T and B lymphocytes are the only lymphoid cells that produce and express specific receptors for antigens.

T Lymphocytes: These cells are involved in the regulation of the immune response and in cell-mediated immunity and help B cells to produce antibodies (humoral immunity). Mature T cells express antigen-specific T cell receptors (TcR) that are clonally segregated (i.e., one cell lineage-one receptor specificity). Every mature T cell also expresses the CD3 molecule, which is associated with the TCR. In addition, mature T cells display one of two accessory molecules, CD4 or CD8. The TCR/CD3 complex recognizes antigens associated with the major histocompatibility complex (MHC) molecules on target cells (e.g. virus-infected cells). The TCR is a transmembrane heterodimer composed of two polypeptide chains (usually, α and β chains). Each chain consists of a constant (C) and a variable (V) region, and is formed by a gene-sorting mechanism similar to that found in antibody formation. The repertoire is generated by the combinatorial joining of variable (V), joining (J), and diversity (D) genes, and by N region (nucleotides inserted by the enzyme deoxynucleotidyl-transferase) diversification. Unlike immunoglobulin genes, genes encoding TcR do not undergo somatic mutation. Thus there is no change in the affinity of the TcR during activation, differentiation, and expansion.

T Helper Cells: These cells are the primary regulators of T cell- and B cell-mediated responses. They 1) aid antigen-stimulated subsets of B lymphocytes to proliferate and differentiate toward antibody-producing cells; 2) express the CD4 molecule; 3) recognize foreign antigen complexed with MHC class II molecules on B cells, macrophages or other antigen-presenting cells; and 4) aid effector T lymphocytes in cell-mediated immunity. Currently, it is believed that there are two functional subsets of T helper (Th) cells. Th1 cells aid in the regulation of cellular immunity, and Th2 cells aid B cells to produce certain classes of antibodies (e.g., IgA and IgE). The functions of these subsets of Th cells depend upon the specific types of cytokines that are generated, for example interleukin-2 (IL-2) and interferon-γ (IFN-γ) by Th1 cells and IL-4 and IL-10 by Th2 cells.

Cell-mediated immunity (delayed hypersensitivity) plays an important role in defense against many intracellular infections such as Mycobacterium tuberculosis. This inflammatory reaction is initiated by the recognition of specific antigens by Th1 cells. Consequently, lymphokines are generated which recruit activated macrophages to eliminate foreign antigens or altered host cells.

T Cytotoxic Cells: These cells are cytotoxic against tumor cells and host cells infected with intracellular pathogens. These cells 1) usually express CD8, 2) destroy infected cells in an antigen-specific manner that is dependent upon the expression of MHC class I molecules.

T Suppressor Cells: These cells suppress the T and B cell responses and express CD8 molecules.

Natural Killer Cells: NK cells are large granular lymphocytes that nonspecifically kill certain types of tumor cells and virus-infected cells. Killing by NK cells is enhanced by cytokines such as IL-2 and IFN-γ. NK cells are also activated by microorganisms to produce a number of cytokines [(IL-2, IFN-γ, IFN-α, and tumor necrosis factor-α (TNF-α)]. These circulating large granular lymphocytes do not express CD3, TCR or immunoglobulin, but display surface receptors (CD16) for the Fc fragment of IgG antibodies.

B Lymphocytes: These cells differentiate into plasma cells to secrete antibodies and are involved in processing proteins and presenting the resultant peptide antigen fragments in the context of MHC molecule to T cells. The genesis of μ and δ chain-positive, mature B cells from pre-B cells is antigen-independent. Pre-B cells in the bone marrow undergo gene rearrangement for IgM heavy (H) chains and consequently express those proteins in the cytoplasm (the μ chain), but no immunoglobulin light (L) chains. B cell development is characterized by recombinations of immunoglobulin H and L chain genes and the expression of specific surface monomeric IgM molecules. At this stage of development, B cells are highly susceptible to the induction of tolerance. Once these cells acquire IgD molecules on their surface, they become mature B cells that are able to differentiate after exposure to antigen into antibody-producing plasma cells.

The activation of B cells into antibody-producing/secreting cells (plasma cells) is antigen-dependent. Once a specific antigen binds to surface Ig molecule, the B cells differentiate into plasma cells that produce and secrete antibodies of the same antigen-binding specificity. If B cells also interact with Th cells, they proliferate and switch the isotype (class) of immunoglobulin that is produced, while retaining the same antigen-binding specificity. This occurs as a result of recombination of the same Ig VDJ genes (the variable region of the Ig) with a different constant (C) region gene such as IgG. In the case of protein antigens, Th2 cells are thought to be required for switching from IgM to IgG, IgA, or IgE isotypes.

IgM is therefore the principal antibody produced during a primary immunization. This primary antibody response is manifested by serum IgM antibodies as early as 3–5 days after the first exposure to an immunogen (immunizing antigen), peaks in 10 days, and persists for some weeks. Secondary or anamnestic antibody responses following repeated exposures to the same antigen appear more rapidly, are of longer duration, have higher affinity, and principally are IgG molecules.

When antibodies bind to antigens, they may 1) neutralize pathogenic features of antigens such as their toxins, 2) facilitate their ingestion by phagocytic cells (opsonization), 3) fix to and activate complement molecules to produce opsonins and chemoattractants (vide infra), or 4) participate in antibody-dependent cellular cytotoxicity (ADCC).

In addition to antibody formation, B cells also process and present protein antigens. After the antigen is internalized it is digested into fragments, some of which are complexed with MHC class II molecules and then presented on the cell surface to CD4⁺ T cells.

Immunoglobulin Supergene Family

Immunoglobulins (Ig)/Antibodies

Immunoglobulins (antibodies) are globular glycoproteins found in body fluids or on B cells where they act as antigen receptors. These molecules are either expressed on the surface of B cells or are secreted by terminally differentiated cells from this lineage (plasma cells) into the circulation or external secretions. An immunoglobulin molecule is an asymmetrical multi-chain peptide consisting of two identical H chains and two identical L chains. Each chain is divided into a V region that is responsible for specific antigen binding and a C region that carries out other functions such as the binding of IgG to complement or leukocytes. These antibody molecules are formed as a result of the assembly of separate germ-line genes for the V, J, and C regions of the H and L chains of the final immunoglobulin molecule. This combinatorial mechanism is responsible for the great diversity of antibody molecules.

There are five major isotypes (classes) of immunoglobulins (IgG, IgA, IgM, IgD, and IgE). These isotypes are distinguished by differences in the C regions of H chains of each immunoglobulin isotype (γ, α, μ, δ, and ε, respectively). These differences are responsible for the particular functions of immunoglobulin classes.

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T Cell Receptor

The specific receptor for antigen on T lymphocytes, the TCR, is a heterodimeric protein with motifs that are similar to immunoglobulin molecules, but whose structure is encoded by a different set of V, J, D, and C genes. Moreover, T cells consist of two subsets carrying different receptors, that have been designated α/β and γ/δ. The T cell receptors act as specific antigen recognition molecules. Unlike antibody molecules, the TcR molecules cannot recognize soluble antigens. In contrast, they recognize protein antigens that have been processed and presented as peptides on the surface of antigen-presenting cells in the context of MHC class I or MHC class II molecules (vide infra).

Major Histocompatibility Complex (MHC)

These genes encode for cell surface molecules that are involved in the genesis and regulation of specific immune responses to T-cell-dependent antigens and in tissue transplantation. They principally encode cell surface protein molecules that bind antigenic peptides, which are recognized by T cells.

The MHC is a cluster of ~ 40–50 genes located on chromosome 6. These genes belong to the super-immunoglobulin gene family. There are three classes of these molecules. MHC class I molecules are found on all nucleated somatic cells and aid in presenting endogenously synthesized antigens, whereas MHC class II molecules are found principally on antigen processing/presenting cells (i.e., macrophages, B cells) and are involved in presenting processed exogenous protein antigens. The MHC class III region contains a heterogeneous group of genes that encode for some components of the complement system, heat shock proteins, tumor necrosis factor-α, and tumor necrosis factor-β.

T Cell Activation

The presentation of antigen in the context of MHC molecules is essential for T cell recognition of peptide antigens. However, interactions between the MHC-bound peptide and TcR and the MHC class I or class II molecules with CD8 or CD4, respectively, are not sufficient to activate T cells. Other ligands on antigen-presenting cells and their receptors (co-receptors/co-stimulators) on T cells are required to complete the process of T cell activation.

Tolerance-Autoimmunity

Immunologic tolerance (unresponsiveness) normally prevents reactions against self-antigens; if immunologic tolerance is broken, autoimmune reactions may occur. Much of the development of tolerance occurs in the thymus by the elimination (clonal deletion) or inactivation (clonal anergy) of self-reactive clones of T cells. Other mechanisms of tolerance occur extrathymically and include activation of antigen-specific T suppressor cells and clonal deletion, which results in the elimination of self-reactive B cells or T cells, and clonal anergy.

Tolerance may be broken because of a genetic predisposition to immune dysregulation, altered self-antigens, exposure to microbial antigens that cross-react with self-antigens, or exposure to a self-antigen that is normally not revealed to the immune system (e.g., an antigen in the eye). When tolerance against self-antigens is broken, autoimmunity is produced, which could result in autoimmune disease.

The Complement System

The complement system consists of inactive circulating glycoproteins that can be sequentially activated by antigen-antibody (IgG or IgM) complexes or bacterial products to enhance inflammation or to attack cellular membranes. The system consists of the classical and alternative pathways that converge to activate the membrane attack complex. After activation, opsonic, chemoattractant, or cytotoxic fragments are produced.

Defenses against Infections

Natural (innate) and acquired defenses are marshaled to combat infecting agents. The first line of defense includes the skin, mucous membranes, protective inhibitors, and IgA antibodies produced at mucosal sites. The second line of defense consists of local factors and cells that are activated or recruited to the site of microbial invasion. These include:

1) the coagulation system,
2) the fibrinolytic system,
3) vasoactive peptides,
4) the complement system,
5) resident macrophages,
6) recruited inflammatory leukocytes, and
7) cytokines.

The third line of defense includes the expansion of populations of antigen-specific B cells and T cells, the production of systemic antibodies, and the activation of T cells. Successful defense is followed by a clearance of opsonized pathogens by the RES and tissue repair.

Immune Responses to Microorganisms Lead to Disease

Excessive or otherwise inappropriate immune responses to infecting agents may lead to disease. Examples of such excessive immunologic responses that can be protective or cause disease include: 1) circulating antigen-antibody (immune) complexes of microbial antigens bound to IgM or IgG antibodies, 2) antibodies to microorganisms that cross-react with self-antigens, 3) vasoactive compounds from the complement system and from the metabolism of arachidonic acid, 4) excessive production of proinflammatory cytokines, 5) delayed hypersensitivity reactions, and 6) cytotoxic T cells directed against the infected host cells.

Ontogeny of the Immune Response

The immune system undergoes an orderly development during the prenatal and postnatal periods. Mature T and B cells appear in the fetus, but are not activated until the infant is exposed to immunogens. Memory T cells are not present during early infancy and the antibody repertoire is not fully established for many months. IgM is the first type of antibody produced postnatally. IgG antibodies to protein antigens are formed in early infancy, but IgG antibodies to polysaccharides do not appear until 2–2.5 years of age. There are also developmental delays in the production of several cytokines such as the interferons.

Maternal Immunologic Contributions to the Infant

Maternal immune factors are transmitted to the fetus via the placenta and to the young infant by mammary gland secretions. These transferred maternal factors compensate for developmental delays in the production of those immune factors by the recipient fetus/infant. Developmental delay in the production of IgG is overcome by the transfer of maternal antibodies of that same isotype via the placenta. Other immune factors (whose production is developmentally delayed), such as secretory IgA, lactoferrin, and lysozyme; leukocytes; anti-inflammatory agents; and immunomodulating agents are provided by mammary gland secretions via human milk. These factors are not as well represented in non-human milk. Therefore, the breast-fed infant is less at risk for gastrointestinal and respiratory infections and for inflammatory disorders including common allergic diseases.

Immunologic Deficiency

Immune deficiencies are genetic or acquired and result in increased susceptibility to certain infections, the types of which depend upon the exact nature of the defect.

Genetic Defects: X-linked agammaglobulinemia is a genetic defect in a B cell progenitor kinase that is essential for B cell development. Consequently, few B cells and only low levels of antibodies are produced. This leads mainly to an increased susceptibility to highly virulent, encapsulated respiratory bacterial infections.

T cell deficiency is the primary problem in severe combined immunodeficiency (deficiencies of B and T cells). Most cases are due to an X-linked recessive defect in the formation of the γ-chain common to a number of cytokine receptors. Some autosomal recessive types are due to deficiencies in enzymes such as adenosine deaminases in the purine salvage pathway. Patients with these diseases display few T cells, decreased T cell functions, poor antibody formation, and increased susceptibility to opportunistic infections such as Pneumocystis carinii.

Hereditary defects also occur in neutrophils. For example, a decrease in leukocyte adherence is due to an autosomal recessive defect in the formation of the common CD18-subunit of leukocyte adherence glycoproteins, whereas deficiency in intracellular killing (chronic granulomatous disease) is due to a deficiency in the production of subunits of cytochrome b₅₅₈ or ancillary proteins necessary for their stabilization. Consequently, reactive oxygen compounds required for intracellular killing are not produced.

Acquired Defects: Protein-energy malnutrition is the leading cause of the immunologic deficiency. A second, but important cause of acquired immunodeficiency is the human immunodeficiency virus (HIV) that attacks CD4⁺ T cells and macrophages. Also, certain other infections depress or destroy parts of the immune system by different mechanisms.

Evolution of the Immune System

The human defense system consists of factors that provide innate and acquired immunity against microorganisms. The system evolved from primitive but effective defenses found in more ancient animal species. The innate defenses include 1) structural barriers, 2) acids, bases, and other chemical agents produced at various sites, such as mucosal surfaces, and 3) highly phagocytic, motile scavenger cells that have well-developed killing and digestive powers. As a result of the evolutionary process, the mammalian immune system has become more specific, efficient, regulated, and complex. The development of specialized innate and acquired recognition/regulatory proteins (antibodies, cell receptors, and cytokines) expanded the repertoire, and control the magnitude of the protective responses. One of the most important consequences of this evolution is the ability of the immune system to discriminate between self and non-self antigens and maintain a memory of previous encounters with antigens, including those from microorganisms.

The evolutionary changes allowed the development of B and T cells which express antigen-specific receptors on their cell surface. These changes permit humans to survive in an environment laden with microbial pathogens and environmental toxins. The pathogenic features of those microorganisms include the ability to

1) enter the body through portals such as the skin, respiratory system, and alimentary tract;
2) utilize nutrients from those sites;
3) adhere to epithelium;
4) produce virulence factors and toxins;
5) commandeer the replicative machinery of the host’s cells;
6) evade the immunologic system;
7) cripple the defenses of the host; and
8) cause autoimmune responses by acting as cross-reactive antigens.

References

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