The tachykinin NK1 receptor mediates the migration-promoting effect of substance P on human skin fibroblasts in culture

Abstract

Fibroblast migration is an important component of the tissue response during the repair process, and substance P (SP) has been shown to exert trophic effects. In the present study, cell migration was evaluated as the distance travelled by adherent human skin fibroblasts (HF) at 96 h and by the number of individual cells moving across a filter within 5 h. In control conditions (1% calf serum) adherent fibroblasts moved from the starting line by approximately 700 μm. The addition of SP (10⁻¹¹–10⁻⁷ M) increased HF mobilisation in a concentration-dependent manner, with maximal activity at 10⁻⁸ M (50% increase in migration over control). Migration of individual HF in suspension was also promoted by SP in a concentration-dependent manner, with an EC₅₀ of 2.2×10⁻⁹ M. The response produced by the maximally effective concentration of SP was equal to 65 and 90% of the effect elicited by 100 ng/ml Platelet-Derived Growth Factor AB (PDGF A/B) on adherent and individual cells respectively. The synthetic NK₁ receptor agonist [Sar⁹]SP-sulphone (10⁻¹¹–10⁻⁶ M) reproduced the SP effect. The NK₂ and NK₃ receptor agonists [βAla⁸]NKA(4–10) and [MePhe⁷]NKB were devoid of any effect. The effect of SP was antagonised by two selective antagonists of NK₁ receptors, namely (±) CP 96,345 (10⁻¹⁰–10⁻⁸ M) and FK 888 (10⁻⁹–10⁻⁷ M), while the NK₂ receptor antagonist MEN 10627 (10⁻⁸–10⁻⁷ M) was not effective. Our data indicate that SP is a potent effector of fibroblast migration and the NK₁ receptor is responsible for this effect. These observations further support the specific role of the NK₁ receptor in mediating the trophic function of SP at the cutaneous level.