Abstract

Abstract Background More than 50% of adults report to suffer from sensitive skin. This common condition is characterized by subjective sensations such as prickling, burning, skin tightness or pruritus, and is often accompanied by objective symptoms like inflammation and erythema. Objective The objective of this study was to develop an active ingredient concept for the treatment of sensitive skin. We tested compounds regarding their potential to (i) decrease the release of proinflammatory mediators, which among others induce erythema and (ii) counteract the hyperresponsiveness of nerve fibres and, thus, exert effects on cutaneous neurosensory dysfunction. Methods 4‐t‐butylcyclohexanol, licochalcone A and acetyl dipeptide‐1 cetyl ester were analysed in vitro regarding their potential to (i) decrease the release of PGE 2 and activation of NF κB and to (ii) inhibit TRPV1 activation or the release of neuronal CGRP. To assess subjective and objective symptoms of skin sensitivity in vivo , two controlled, single‐blind, randomized studies were conducted with 4‐t‐butylcyclohexanol and the combination with licochalcone A. Results In vitro , 4‐t‐butylcyclohexanol significantly reduced TRPV 1 activation, while acetyl dipeptide‐1 cetyl ester had no effect on receptor activation. Licochalcone A significantly decreased NF κB signalling and PGE 2 secretion, at lower concentrations than acetyl dipeptide‐1 cetyl ester. A formulation containing 4‐t‐butylcyclohexanol showed a significant immediate anti‐stinging/anti‐burning effect in vivo , and a cream base containing a combination of 4‐t‐butylcyclohexanol and a licochalcone A‐rich licorice extract reduced shaving‐induced erythema. Conclusion In vitro and in vivo data indicate that the combination of the TRPV 1 antagonist 4‐t‐butylcyclohexanol and the potent anti‐inflammatory licochalcone A provide an effective active ingredient concept for the treatment of sensitive skin, as the topical application resulted in an immediate relief from symptoms such as erythema and stinging.