Increased anti‐oxidative action compensates for collagen tissue degeneration in vitiligo dermis

Author:

Yokoi Kazunori1ORCID,Yasumizu Yoshiaki2ORCID,Ohkura Naganari2ORCID,Shinzawa Koei3ORCID,Okuzaki Daisuke4ORCID,Shimoda Nene5ORCID,Ando Hideya5ORCID,Yamada Nanako6ORCID,Fujimoto Manabu1ORCID,Tanemura Atsushi1ORCID

Affiliation:

1. Department of Dermatology Osaka University Graduate School of Medicine Osaka Japan

2. Department of Experimental Immunology, Immunology Frontier Research Center, Faculty of Medicine Osaka University Osaka Japan

3. Departments of Molecular Biology and Biochemistry Osaka University Graduate School of Medicine Osaka Japan

4. Genome Information Research Center, Research Institute for Microbial Diseases Osaka University Osaka Japan

5. Department of Applied Chemistry and Biotechnology Okayama University of Science Okayama Japan

6. Division of Dermatology, Department of Medicine of Sensory and Motor Organs, Faculty of Medicine Tottori University Tottori Japan

Abstract

AbstractVitiligo is a common depigmentation disorder characterized by the selective loss of melanocytes. In our daily clinic experience, we noticed that the skin tightness of hypopigmented lesions would be more evident in comparison to that of uninvolved perilesional skin in vitiligo patients. Therefore, we hypothesized that collagen homeostasis might be maintained in vitiligo lesions, irrespective of the substantial excessive oxidative stress that occurs in association with the disease. We found that the expression levels of collagen‐related genes and anti‐oxidative enzymes were upregulated in vitiligo‐derived fibroblasts. Abundant collagenous fibers were observed in the papillary dermis of vitiligo lesions in comparison to uninvolved perilesional skin by electron microscopy. The production of matrix metalloproteinases that degraded collagen fibers was suppressed. The deposition of acrolein adduct protein, which is a product of oxidative stress, was significantly reduced in vitiligo dermis and fibroblasts. As part of the mechanism, we found upregulation of the NRF2 signaling pathway activity, which is an important defense system against oxidative stress. Taken together, we demonstrated that the anti‐oxidative action and collagen production were upregulated and that the collagen degeneration was attenuated in vitiligo dermis. These new findings may provide important clues for the maintenance of antioxidant ability in vitiligo lesions.

Publisher

Wiley

Subject

Dermatology,General Biochemistry, Genetics and Molecular Biology,Oncology

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