International Journal of Molecular Sciences (Apr 2024)

Thymic Stromal Lymphopoietin (TSLP) Is Cleaved by Human Mast Cell Tryptase and Chymase

  • Luisa Canè,
  • Remo Poto,
  • Francesco Palestra,
  • Ilaria Iacobucci,
  • Marinella Pirozzi,
  • Seetharaman Parashuraman,
  • Anne Lise Ferrara,
  • Amalia Illiano,
  • Antonello La Rocca,
  • Edoardo Mercadante,
  • Piero Pucci,
  • Gianni Marone,
  • Giuseppe Spadaro,
  • Stefania Loffredo,
  • Maria Monti,
  • Gilda Varricchi

DOI
https://doi.org/10.3390/ijms25074049
Journal volume & issue
Vol. 25, no. 7
p. 4049

Abstract

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Thymic stromal lymphopoietin (TSLP), mainly expressed by epithelial cells, plays a central role in asthma. In humans, TSLP exists in two variants: the long form TSLP (lfTSLP) and a shorter TSLP isoform (sfTSLP). Macrophages (HLMs) and mast cells (HLMCs) are in close proximity in the human lung and play key roles in asthma. We evaluated the early proteolytic effects of tryptase and chymase released by HLMCs on TSLP by mass spectrometry. We also investigated whether TSLP and its fragments generated by these enzymes induce angiogenic factor release from HLMs. Mass spectrometry (MS) allowed the identification of TSLP cleavage sites caused by tryptase and chymase. Recombinant human TSLP treated with recombinant tryptase showed the production of 1-97 and 98-132 fragments. Recombinant chymase treatment of TSLP generated two peptides, 1-36 and 37-132. lfTSLP induced the release of VEGF-A, the most potent angiogenic factor, from HLMs. By contrast, the four TSLP fragments generated by tryptase and chymase failed to activate HLMs. Long-term TSLP incubation with furin generated two peptides devoid of activating property on HLMs. These results unveil an intricate interplay between mast cell-derived proteases and TSLP. These findings have potential relevance in understanding novel aspects of asthma pathobiology.

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