Utilizza questo identificativo per citare o creare un link a questo documento: http://elea.unisa.it/xmlui/handle/10556/4479
Titolo: The urokinase/urokinase receptor system in mast cells: effects of its functional interaction with fmlf receptors
Autore: Rossi, Francesca Wanda
Prevete, Nella
Rivellese, Felice
Napolitano, Filomena
Montuori, Nunzia
Postiglione, Loredana
Selleri, Carmine
De Paulis, Amato
Parole chiave: Mast Cells;FPRs;uPA/uPAR;VEGF-A
Data: 2016
Citazione: Rossi FW, Prevete N, Rivellese F, Napolitano F, Montuori N, Postiglione L, Selleri C, de Paulis A. The urokinase/urokinase receptor system in mast cells: effects of its functional interaction with fmlf receptors. Translational Medicine @ UniSa 2016, 15(5): 34-41.
Abstract: Mast cell and basophils express the high affinity receptor for IgE (FcRI) and are primary effector cells of allergic disorders. The urokinase (uPA)-mediated plasminogen activation system is involved in physiological and pathological events based on cell migration and tissue remodelling, such as inflammation, wound healing, angiogenesis and metastasis. uPA is a serine protease that binds uPAR, a high affinity glycosyl-phosphatidyl-inositol (GPI)- anchored receptor. uPAR focuses uPA activity at the cell surface and activates intracellular signaling through lateral interactions with integrins, receptor tyrosine kinases and the G-protein-coupled family of fMLF chemotaxis receptors (FPRs). We investigated the expression of the uPAuPAR system and its functional interaction with FPRs in human mast cells (MCs). Differently from basophils, MCs produced uPA that was able to induce their chemotaxis. Indeed, MCs also expressed uPAR, both in the intact and in a cleaved form (DIIDIII-uPAR) that can expose, at the N-terminus, the SRSRY sequence, able to interact with FPRs and to mediate cell chemotaxis. MCs also expressed mRNAs for FPRs that were functionally active; indeed, uPA and a soluble peptide (uPAR84-95), containing the SRSRY chemotactic sequence of uPAR and able to interact with FPRs, were able to induce MCs chemotaxis. Thus, uPA is a potent chemoattractant for MCs acting through the exposure of the chemotactic epitope of uPAR, that is an endogenous ligand for FPRs. The same mechanism could be involved in VEGF-A secretion by human MCs, also induced by uPA and uPAR84-95 stimulation.
URI: http://www.translationalmedicine.unisa.it/index
http://elea.unisa.it:8080/xmlui/handle/10556/4479
http://dx.doi.org/10.14273/unisa-2677
ISSN: 2239-9747
È visualizzato nelle collezioni:Translational Medicine @ UniSa. Volume 15 (may. - aug. 2016)

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