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Why the 20% + 2 tryptase formula is a diagnostic gold standard for severe systemic mast cell activation and mast cell activation syndrome
JournalArticle (Originalarbeit in einer wissenschaftlichen Zeitschrift)
ID
4510241
Author(s)
Valent, Peter; Bonadonna, Patrizia; Hartmann, Karin; Broesby-Olsen, Sigurd; Brockow, Knut; Butterfield, Joseph H.; Triggiani, Massimo; Lyons, Jonathan J.; Oude Elberink, Joanna N. G.; Arock, Michel; Metcalfe, Dean D.; Akin, Cem
Anaphylaxis, diagnosis; Biomarkers; Humans; Mast Cells, immunology; Mastocytosis, immunology; Reference Values; Reproducibility of Results; Sensitivity and Specificity; Tryptases, blood
Abstract
Mast cell activation syndrome (MCAS) is a condition characterized by recurrent episodes of clinically relevant, systemic, severe reactions to mast cell (MC)-derived mediators released in the context of anaphylaxis or another acute MC-related event. It is important to document MC involvement in these reactions in order to establish the diagnosis MCAS. The most specific and reliable marker of systemic MC activation is an acute and substantial event-related (transient) increase in the serum tryptase level over the individual's baseline value. However, the baseline level of tryptase varies depending on the underlying disease and the genetic background. For example, an estimated 3-5% of healthy individuals exhibit duplications or multiple copies of the TPSAB1 gene encoding for alpha-tryptase, and over 30% of all patients with myeloid neoplasms, including mastocytosis, have elevated basal tryptase levels. Therefore, it is of utmost importance to adjust the event-related diagnostic (MCAS-confirming) increase in tryptase over the individual baseline in a robust approach. To address this challenge, the 20% + 2 formula was proposed by the consensus group in 2012. Since then, this approach has been validated in clinical practice by independent groups and found to be sound. In the current article, we discuss the emerging importance and value of the 20% + 2 formula in clinical practice and its role as a criterion of severe systemic MC activation and MCAS.
