Science and Research

Mast cells as protectors of health

Mast cells (MC), well known for their effector functions in Th2 skewed allergic and also autoimmune inflammation, become increasingly acknowledged for their role in protection of health. It is now clear that they are also key modulators of immune responses at interface organs like skin or gut. MC can prime tissues for adequate inflammatory responses and cooperate with dendritic cells in T cell activation. They also regulate harmful immune responses in trauma and help to successfully orchestrate pregnancy. This review focusses on the beneficial effects of mast cells on tissue homeostasis and elimination of toxins or venoms. MC can enhance pathogen clearance in many bacterial, viral, and parasite infections, e.g. by TLR2 triggered degranulation, secretion of antimicrobial cathelicidins, recruiting neutrophils or by providing extracellular DNA traps. The role of MC in tumors is more ambiguous, however, encouraging new findings show they can change the tumor microenvironment towards anti-tumor immunity when adequately triggered. Uterine tissue remodeling by alpha-chymase (MCP-5) is crucial for successful embryo implantation. MCP-4 and the tryptase MCP-6 emerge to be protective in CNS trauma by reducing inflammatory damage and excessive scar formation, thereby protecting axon growth. Last but not least, we see proteases like carboxypeptidase A released by FcepsilonRI activated MC detoxify an increasing number of venoms and endogenous toxins. A better understanding of the plasticity of MC will help to improve these advantageous effects, and hint on ways to cut down detrimental MC actions.

  • Dudeck, A.
  • Koberle, M.
  • Goldmann, O.
  • Meyer, N.
  • Dudeck, J.
  • Lemmens, S.
  • Rohde, M.
  • Roldan, N. G.
  • Dietze-Schwonberg, K.
  • Orinska, Z.
  • Medina, E.
  • Hendrix, S.
  • Metz, M.
  • Zenclussen, A. C.
  • von Stebut, E.
  • Biedermann, T.

Keywords

  • CNS trauma
  • infection
  • innate immunity
  • mast cell
  • mast cell protease
  • pregnancy
  • toxin
  • tumor
  • venom
Publication details
DOI: 10.1016/j.jaci.2018.10.054
Journal: The Journal of allergy and clinical immunology
Work Type: Original
Location: ARCN
Disease Area: AA
Partner / Member: FZB
Access-Number: 30468774
See publication on PubMed

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