An introduction to immunology and immunopathology
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- Fig. 1 Characteristics and function of cells involved in innate immunity
- Adaptive immunity
- T cells and APCs
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Cell
Image % in adults Nucleus Functions Lifetime Main targets Macrophage* Varies Varies
• Phagocytosis • Antigen
presentation to T cells
Months – years • Various Neutrophil 40-75%
Multi-lobed • Phagocytosis • Degranulation (discharge of contents of a cell) 6 hours – few days
• Bacteria
• Fungi
Eosinophil 1-6%
Bi-lobed • Degranulation • Release of enzymes, growth factors, cytokines 8-12 days (circulate for 4-5 hours) •
• Various allergic tissues Basophil
< 1% Bi- or tri-lobed • Degranulation • Release of histamine, enzymes, cytokines Lifetime uncertain; likely a few hours – few days • Various allergic tissues Mast cell Common in tissues Central, single- lobed •
• Release of histamine, enzymes, cytokines Months to years • Parasites • Various allergic tissues Lymphocytes (T cells) 20-40%
Deeply staining, eccentric T helper (Th) cells (CD4+): immune response mediators Cytotoxic T cells (CD8+): cell destruction Weeks to years • Th cells: intracellular bacteria • Cytotoxic T cells: virus infected and tumour cells • Natural killer cells: virus-infected and tumour cells Monocyte 2-6%
Kidney shaped Differentiate into macrophages and dendritic cells to elicit an immune response Hours – days • Various
Natural killer (NK) cell
15% (varies) of circulating lymphocytes and tissues
Single-lobed • Tumour rejection • Destruction of infected cells • Release of perforin and granzymes which induce apoptosis 7-10 days • Viruses
• Tumour cells Fig. 1 Characteristics and function of cells involved in innate immunity [ 1 , 3 , 4 ]. *Dust cells (within pulmonary alveolus), histiocytes (connective tissue), Kupffer cells (liver), microglial cells (neural tissue), epithelioid cells (granulomas), osteoclasts (bone), mesangial cells (kidney) Page 8 of 14 Marshall et al. Allergy Asthma Clin Immunol 2018, 14(Suppl 2):49 immune response to specific pathogens and contribute to immune regulation in that tissue. The main characteristics and functions of the cells involved in the innate immune response are summarized in Fig. 1 . Adaptive immunity The development of adaptive immunity is aided by the actions of the innate immune system, and is critical when innate immunity is ineffective in eliminating infectious agents. The primary functions of the adaptive immune response are: the recognition of specific “non- self” antigens, distinguishing them from “self” antigens; the generation of pathogen-specific immunologic effector pathways that eliminate specific pathogens or pathogen-infected cells; and the development of an immunologic memory that can quickly eliminate a specific pathogen should subsequent infections occur [ 2 ].
Adaptive immune responses are the basis for effective immunization against infectious diseases. The cells of the adaptive immune system include: antigen-specific T cells, which are activated to proliferate through the action of APCs, and B cells which differentiate into plasma cells to produce antibodies. T cells and APCs T cells derive from hematopoietic stem cells in bone marrow and, following migration, mature in the thymus. These cells express a series of unique antigen-binding receptors on their membrane, known as the T-cell receptor (TCR). Each T cell expresses a single type of TCR and has the capacity to rapidly proliferate and differentiate if it receives the appropriate signals. As previously mentioned, T cells require the action of APCs (usually dendritic cells, but also macrophages, B cells, fibroblasts and epithelial cells) to recognize a specific antigen.
The surfaces of APCs express a group of proteins known as the major histocompatibility complex (MHC). MHC are classified as either class I (also termed human leukocyte antigen [HLA] A, B and C) which are found on all nucleated cells, or class II (also termed HLA DP, DQ and DR) which are found only on certain cells of the immune system, including macrophages, dendritic cells and B cells. Class I MHC molecules present endogenous (intracellular) peptides, while class II molecules on APCs present exogenous (extracellular) peptides to T cells. The MHC protein displays fragments of antigens (peptides) when a cell is infected with an intracellular pathogen, such as a virus, or has phagocytosed foreign proteins or organisms [ 2 ,
]. T cells have a wide range of unique TCRs which can bind to specific foreign peptides. During the development of the immune system, T cells that would react to antigens normally found in our body are largely eliminated. T cells are activated when they encounter an APC that has digested an antigen and is displaying the correct antigen fragments (peptides) bound to its MHC molecules. The opportunities for the right T cells to be in contact with an APC carrying the appropriate peptide MHC complex are increased by the circulation of T cells throughout the body (via the lymphatic system and blood stream) and their accumulation (together with APCs) in lymph nodes. The MHC-antigen complex activates the TCR and the T cell secretes cytokines which further control the immune response. This antigen presentation process stimulates T cells to differentiate primarily into either cytotoxic T cells (CD8+ cells) or T-helper (Th) cells (CD4+ cells) (see Fig. 2 ). CD8+ cytotoxic T cells are primarily involved in the destruction of cells infected by foreign agents, such as viruses, and the killing of tumour cells expressing appropriate antigens. They are activated by the interaction of their TCR with peptide bound to MHC class I molecules. Clonal expansion of cytotoxic T cells produces effector cells which release substances that induce apoptosis of target cells. Upon resolution of the infection, most effector cells die and are cleared by phagocytes. However, a few of these cells are retained as memory cells that can quickly differentiate into effector cells upon subsequent encounters with the same antigen [ 2 , 3 ]. CD4+ Th cells play an important role in establishing and maximizing the immune response. These cells have no cytotoxic or phagocytic activity, and cannot directly kill infected cells or clear pathogens. However, they “mediate” the immune response by directing other cells to perform these tasks and regulate the type of immune response that develops. Th cells are activated through TCR recognition of antigen bound to class II MHC molecules. Once activated, Th cells release cytokines that influence the activity of many cell types, including the APCs that activate them. Several types of Th cell responses can be induced by an APC, with Th1, Th2 and Th17 being the most frequent. The Th1 response is characterized by the production of IFN-γ which activates the bactericidal activities of macrophages and enhances anti-viral immunity as well as immunity to other intracellular pathogens. Th1- derived cytokines also contribute to the differentiation of B cells to make opsonizing antibodies that enhance the efficiency of phagocytes. An inappropriate Th1 response is associated with certain autoimmune diseases. The Th2 response is characterized by the release of cytokines (IL-4, 5 and 13) which are involved in the development of immunoglobulin E (IgE) antibody- producing B cells, as well as the development and
Page 9 of 14 Marshall et al. Allergy Asthma Clin Immunol 2018, 14(Suppl 2):49 recruitment of mast cells and eosinophils that are essential for effective responses against many parasites. In addition, they enhance the production of certain forms of IgG that aid in combatting bacterial infection. As mentioned earlier, mast cells and eosinophils are instrumental in the initiation of acute inflammatory responses, such as those seen in allergy and asthma. IgE antibodies are also associated with allergic reactions (see Table 2 ). Therefore, an imbalance of Th2 cytokine production is associated with the development of atopic (allergic) conditions. Th17 cells have been more recently described. They are characterized by
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