| Literature DB >> 33445787 |
Leonardo Cristinziano1,2, Remo Poto1,2, Gjada Criscuolo1,2,3, Anne Lise Ferrara1,2,4, Maria Rosaria Galdiero1,2,3,4, Luca Modestino1,2, Stefania Loffredo1,2,3,4, Amato de Paulis1,2,3, Gianni Marone1,2,3,4, Giuseppe Spadaro1,2,3, Gilda Varricchi1,2,3,4.
Abstract
Human lung mast cells (HLMCs) express the high-affinity receptor FcεRI for IgE and are strategically located in different compartments of <span class="Species">human lung, where they play a role in several inflammatory disorders and cancer. Immunoglobulin superantigens (e.g., protein A of Staphylococcus aureus and protein L of Peptostreptococcus magnus) bind to the variable regions of either the heavy (VH3) or light chain (κ) of IgE. IL-33 is a cytokine expressed by epithelial cells that exerts pleiotropic functions in the lung. The present study investigated whether immunoglobulin superantigens protein A and protein L and IL-33 caused the release of inflammatory (histamine), angiogenic (VEGF-A) and lymphangiogenic (VEGF-C) factors from HLMCs. The results show that protein A and protein L induced the rapid (30 min) release of preformed histamine from HLMCs. By contrast, IL-33 did not induce the release of histamine from lung mast cells. Prolonged incubation (12 h) of HLMCs with superantigens and IL-33 induced the release of VEGF-A and VEGF-C. Preincubation with IL-33 potentiated the superantigenic release of histamine, angiogenic and lymphangiogenic factors from HLMCs. Our results suggest that IL-33 might enhance the inflammatory, angiogenic and lymphangiogenic activities of lung mast cells in pulmonary disorders.Entities:
Keywords: IL-33; VEGF-A; VEGF-C; allergy; asthma; histamine; mast cell; protein A; protein L; superantigen
Year: 2021 PMID: 33445787 PMCID: PMC7828291 DOI: 10.3390/cells10010145
Source DB: PubMed Journal: Cells ISSN: 2073-4409 Impact factor: 6.600