Mast cell

Author: Prof. Dr. med. Peter Altmeyer

All authors of this article

Last updated on: 15.04.2023

Dieser Artikel auf Deutsch

Definition
This section has been translated automatically.

Mast cells have been so named (after Paul Ehrlich) because they look like "fattened" under the light microscope. Mast cells are characterized by their staining with basophilic dyes (toluidine blue; tolonium chloride) and a granular cytoplasm.

Mast cells are amoeboid mobile, small tissue cells, which are mainly found in the connective tissue (connevtive tissue mast cells, CTMC, tissue mast cells) of humans and vertebrates of the skin, intestine and lungs (mucosa mast cells).

Mast cells are predominantly perivascular in the tissue. It has been shown that they have direct access to the bloodstream. They penetrate the vascular lumen with cell extensions and perform a kind of guard function there by randomly checking the blood stream for its content. In doing so they "fish" for free IgE antibodies (Cheng 2013).

General information
This section has been translated automatically.

Mast cells belong to the innate immunity of the immune system. The physiological tasks of mast cells include the immediate defense against infections at the interfaces of the body with its environment. Mast cells contain numerous mediators which are stored in 0.5-0.8 µm large vesicles visible under the light microscope as granules (mast cell granules). One mast cell contains about 500 such vesicles. These contain histamine, heparin and serotonin, among other substances. In addition, mast cells as well as basophilic granulocytes produce mediators such as PAF, prostaglandin D2 and leukotrienes (LTC4, LTD4, LTE4) as well as tumor necrosis factor. Degranulation and exocytosis with release of the mediators is mediated, for example, in a type I reaction via high-affinity IgE receptors on the cell surface. This reaction occurs when these receptors are cross-linked by IgE-bound allergens.

Mast cells, like basophilic granulocytes, develop in the bone marrow from oligopotent CD34 + myeloid stem cells. Such stem cells, under certain conditions, mature into cells that differentiate into basophilic granulocytes of the blood.

Tissue mast cells: The immature progenitor cells of tissue mast cells enter the connective tissues of their end organs, mucous membranes and skin via blood vessels. These cells express the tyrosine kinase receptor KIT (CD117), which binds stem cell factor (SCF). SCF is a growth factor essential for proliferation and differentiation of mast cells. In the tissue of their end organs, the immature cells differentiate into mature mast cells. Mutations leading to a defect of SCF or KIT result in mast cell deficiency. An activating KIT D816 mutation (>95% KIT D816V in exon 17) is detectable in 80-95% of patients with systemic mastocytosis and leads to SCF-independent receptor activation with clonal expansion and accumulation of tissue mast cells.Other growth factors for mast cells are mainly IL-3 (interleukin-3), IL-5 (interleukin-5) and GM-CSF.

Mast cells interact with other leukocytes and play an important role in the complex initiation and control of allergic reactions as well as in the defense against parasites. For example, mast cells form a functional unit with basophilic granulocytes and induce IgE synthesis in plasma cells. Remarkably, basophilic granulocytes in humans are much more sensitive to allergic reactions than mast cells, which are much more abundant.

Mast cell activation is critical for the induction of cutaneous inflammatory response in the context of allergic, autoimmunologic, and infectious skin diseases. An activated mast cell secretes its mediators. A total of > 200 mast cell mediators have been identified to date. With this mediator release, the mast cells cause invading infectious agents to be acutely and directly attacked and eliminated without the need for further processes of an immune cascade. In these defense mechanisms, the mast cell does not follow an "all or nothing" response. Rather, the response of the mast cells to the activating stimulus varies depending on the type and intensity of the stimulus. Mediator release is either slow and continuous or explosive (e.g., following antigen contact). When release is slow due to weak stimuli, the mast cell appears to remain intact. In contrast, when the stimulus is strong, the cell membrane dissolves completely. The mast cell disintegrates abruptly. The granules are released and dissolve.

Furthermore, chemical and physical stimuli (e.g. pressure in urticaria factitia) are known to cause a non-specific release of their mediators (without antigen-antibody reaction) in mast cells which is not triggered by an immune reaction. Such reactions are the pathophysiological basis of apseudoallergic reaction(pseudoallergy).

The various mediators of mast cells cause the migration of other immune cells, such as neutrophils or eosinophilic granulocytes to the site of inflammation. The released mediators first enter the intercellular spaces, where they bind to their specific receptors on the surfaces of the surrounding cells. They are rapidly degraded after their release, even before they can enter the lymph or bloodstream. Only when the amount of mediators released exceeds the local binding and degradation capacity can they trigger systemic reactions (e.g. anaphylactic reactions).

Furthermore, mast cells are antigen-presenting cells. They can induce and enhance specific immune responses. For example, the targeted immune response is via the high-affinity FcεRI receptor. When two IgE antibodies on the surface of the mast cell cross-link with a matching antigen (e.g., parasite or foreign substance or allergen) (antigen-antibody complex), this cross-linking triggers a biochemical signal that leads to activation of the mast cell.

The following receptors could be detected on mast cells and activate them:

  • Antibody receptors (Fc receptors) IgA, and IgG antibodies (the role of IgA antibody receptors is not yet clear.
  • IgG: stimulation or inhibition of mast cell activity, depending on the receptor.
  • Toll-like receptors (TLR1-9 ): Activation by bacterial products
  • Histamine receptors (H1, H2, H4 ): Mast cell activation
  • Serotonin receptors (5-HT1A ): Adhesion (adherence), chemotaxis (migration).
  • Kit receptor(tyrosine kinase receptor - CD117)
  • Stem cell factor: Mast cell activation
  • Beta2-adrenoceptor: inhibition of mast cell degranulation in allergic reactions
  • Estrogen receptor: Enhanced release of mediators
  • Progesterone receptor: Inhibition of mediator release
  • Prostaglandin E receptor ( EP2, EP3, EP4): Inhibition of IgE antibody-mediated eicosanoid production and mediator release.
  • Receptors for neuropeptides (e.g. substance P): Degranulation of mast cells may occur via nerve stimuli.
  • Vitamin D3 receptors: Stimulation of vitamin D3 receptors has a stabilizing effect on mast cells. Vitamin D3 deficiency increases mast cell activation.
  • Cannabinoid receptor: Suppresses mast cell activity.
  • Leptin receptors: Immunomodulatory effects
  • Protease-activated receptor (PAR1-4 serine proteases - e.g. trypsin, tryptase): Mast cell activation with mediator release

Note(s)
This section has been translated automatically.

The total mass of mast cells in the organism corresponds approximately to an organ the size of the spleen. CTMCs from different tissues differ from those of the skin in the size of the granules, their functions, stainability and phamacological properties.

In humans, mucosal mast cells (MMCs) are mainly found in the midgut and lungs. Their number increases significantly during a parasitic infection. Mast cells are found in the nasal mucosa in allergic rhinitis. Their number is drastically reduced by local corticosteroids.

The mucosa contains an abundance of mast cells or their precursors. In the duodenal mucosa there are 20,000 mast cells mm3, which is three times as much as in the outer skin (Barret et al. 1984). In newborns the number is still small. It rises in the laudfe of life to fall again in old age.

The cells circulating in the blood analogous to CTMCs are called basophilic granulocytes.

Literature
This section has been translated automatically.

  1. Barrett KE et al (1984) The mucosal mast cell and is role in gastointestinal allergic diseases. Clin Rev Allergy 2: 39-53.
  2. Cheng LE et al (2013) Perivascular mast cells dynamically probe cutaneous blood vessels to capture immunoglobulin E. Immunity 38:166-75.
  3. Suurmond J et al (2016) Mast cells in rheumatic disease. Eur J Pharmacol 778:116-124.
  4. Taildeman J et al (2009) Human mast cells express leptin and leptin receptors. Histochem Cell Biol 131:703-711.
  5. Toniato E et al (2015) IMMUNOMODULATORY EFFECTS OF VITAMIN D ON SKIN INFLAMMATION. J Biol Regul Homeost Agents 29:563-567
  6. Suurmond J et al(2015) Differential TLR-induced cytokine production by human mast cells is amplified by FcɛRI triggering. Clin Exp Allergy 45:788-796.
  7. Yu et al.(2015) Non-IgE mediated mast cell activation. Eur J Pharmacoldoi: 10.1016/j.ejphar.2015.07.017.
  8. Wu H et al (2015) The Origin, Expression, Function and Future Research Focus of a G Protein-coupled Receptor, Mas-related Gene X2 (MrgX2)"Prog Histochem Cytochem doi: 10.1016/j.proghi.2015.06.001.
  9. Zuo L et al (2015) Molecular Regulation of Toll-like Receptors in Asthma and COPD. Front Physiol 6:312.

Authors

Last updated on: 15.04.2023