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Functional Expression of Neurokinin 1 Receptors on Mast Cells Induced by IL-4 and Stem Cell Factor¹

Hanneke P. M. van der Kleij^2,*, Donglai Ma, Frank A. M. Redegeld^*, Aletta D. Kraneveld^*, Frans P. Nijkamp^* and John Bienenstock

^* Department of Pharmacology and Pathophysiology, Utrecht Institute for Pharmaceutical Sciences, Utrecht University, Utrecht, The Netherlands; and Department of Pathology and Molecular Medicine, McMaster University, Hamilton, Ontario, Canada

It is widely accepted that neurokinin 1 (NK₁) receptors are not generally expressed on mast cells but little is known about their expression in inflammation. The present study shows expression of NK₁ receptors on bone marrow-derived mast cells (BMMC) under the influence of IL-4 or stem cell factor (SCF). Highest expression was found when both cytokines are present. Six days of coculture with the cytokines IL-4 and SCF showed significant expression of NK₁ receptors (NK₁ receptor⁺/c-kit⁺ BMMC; control: 7%, IL-4/SCF: 16%), while 12 days of cytokine coculture increased this expression to 37% positive cells. A longer coculture with IL-4 and SCF did not give an additional effect. Increased expression in IL-4/SCF-treated BMMC was further confirmed using Western blot analysis. Next, we demonstrated the functional relevance of NK₁ receptor expression for mast cell activation, resulting in an enhanced degranulation upon stimulation by substance P. BMMC activation was significantly diminished by the NK₁ receptor antagonist RP67580 (10 µM) when stimulated with low concentrations of substance P. The inactive enantiomer RP65681 had no effect. In addition, BMMC cultured from bone marrow of NK₁ receptor knockout mice showed significantly decreased exocytosis to low concentrations of substance P. The present study clearly shows that NK₁ receptor-induced activation contributes significantly at low physiological substance P concentrations (<100 µM). In conclusion, BMMC were shown to express NK₁ receptors upon IL-4/SCF coculture. This expression of NK₁ receptors has been demonstrated to be of functional relevance and leads to an increase in the sensitivity of BMMC to substance P.

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