Cytoglobin functions as a redox regulator of melanogenesis in normal epidermal melanocytes

Author:

Tanaka Yo1ORCID,Sato‐Matsubara Misako23ORCID,Tsuruta Daisuke4ORCID,Tanaka Hiroshi1ORCID,Kadono Chiho3ORCID,Sugawara Koji4ORCID,Kawada Norifumi2ORCID,Wakamatsu Kazumasa5ORCID,Ito Shosuke5ORCID,Yoshizato Katsutoshi3ORCID

Affiliation:

1. Research Laboratories Nippon Menard Cosmetic Co., Ltd. Nagoya Japan

2. Department of Hepatology, Graduate School of Medicine Osaka Metropolitan University Osaka Japan

3. Donated Synthetic Biology Laboratory Osaka Metropolitan University Graduate School of Medicine Osaka Japan

4. Department of Dermatology Osaka Metropolitan University Graduate School of Medicine Osaka Japan

5. Institute for Melanin Chemistry Fujita Health University Toyoake Japan

Abstract

AbstractEpidermal melanocytes are continuously exposed to sunlight‐induced reactive oxygen species (ROS) and oxidative stress generated during the synthesis of melanin. Therefore, they have developed mechanisms that maintain normal redox homeostasis. Cytoglobin (CYGB), a ubiquitously expressed intracellular iron hexacoordinated globin, exhibits antioxidant activity and regulates the redox state of mammalian cells through its activities as peroxidase and nitric oxide (NO) dioxygenase. We postulated that CYGB functions in the melanogenic process as a regulator that maintains oxidative stress within a physiological level. This was examined by characterizing normal human melanocytes with the knockdown (KD) of CYGB using morphological and molecular biological criteria. CYGB‐KD cells were larger, had more dendrites, and generated more melanin granules in the advanced stages of melanogenesis than control cells. The expression levels of major melanogenesis‐associated genes and proteins were higher in CYGB‐KD melanocytes than in wild type (WT) cells. As expected, CYGB‐KD melanocytes generated more ROS and NO than WT cells. In conclusion, CYGB physiologically contributes to maintaining redox homeostasis in the melanogenic activity of normal melanocytes by controlling the intracellular levels of ROS and NO.

Publisher

Wiley

Subject

Dermatology,General Biochemistry, Genetics and Molecular Biology,Oncology

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