Sodium dl‐ α ‐ tocopheryl phosphate inhibits ultraviolet‐induced production of reactive nitrogen species in human keratinocytes

It has been well established that UV irradiation causes various kinds of photodamage in human skin. Skin photodamage is mainly caused by reactive oxygen species (ROS), such as superoxide, hydroxyl radical, hydrogen peroxide, and singlet oxygen. Recently, it has been revealed that reactive nitrogen species (RNS), such as nitric oxide (NO) and peroxynitrite (ONOO − ), are also an important consideration in UV‐irradiated human skin. Reactive nitrogen species cause several types of skin damage, for example erythema, darkening, disruption of epidermal barrier function, and psoriasis. Therefore, it is very important to control RNS production for beautiful skin to be maintained. However, RNS are indirectly measured by stable degradation products because their life is very short. In this present study, we attempted the direct observation of RNS production in human keratinocytes. As a result, we succeeded in direct measurement of real‐time UVB‐induced RNS production in human keratinocytes by using a RNS‐specific fluorescence probe. On the other hand, sodium dl ‐α‐tocopheryl phosphate (VEP), a newly synthesized water‐soluble vitamin E derivative, inhibited UVB‐induced RNS production in human keratinocytes. Furthermore, we revealed that UVB‐induced neuronal nitric oxide synthase (nNOS) mediates RNS production in human keratinocytes. These results suggest that VEP is a useful ingredient for cosmetic products, and that VEP may protect the skin from several kinds of damage caused by UV‐induced RNS production. Key words:  sodium dl ‐α‐tocopheryl phosphate (VEP), reactive nitrogen species (RNS), nitric oxide (NO), peroxynitrite (ONOO − ), neuronal nitric oxide synthase (nNOS), RNS‐specific fluorescence probe, UV, keratinocytes, reactive oxygen species (ROS), skin photodamage.