Novel UV‐B Phototherapy With a Light‐Emitting Diode Device Prevents Atherosclerosis by Augmenting Regulatory T‐Cell Responses in Mice

Author:

Tanaka Toru1ORCID,Sasaki Naoto12ORCID,Krisnanda Aga1ORCID,Shinohara Masakazu34ORCID,Amin Hilman Zulkifli156ORCID,Horibe Sayo1ORCID,Ito Ken1ORCID,Iwaya Motoaki7ORCID,Fukunaga Atsushi8ORCID,Hirata Ken‐ichi2,Rikitake Yoshiyuki1ORCID

Affiliation:

1. Laboratory of Medical Pharmaceutics Kobe Pharmaceutical University Kobe Japan

2. Division of Cardiovascular Medicine, Department of Internal Medicine Kobe University Graduate School of Medicine Kobe Japan

3. Division of Molecular Epidemiology Kobe University Graduate School of Medicine Kobe Japan

4. The Integrated Center for Mass Spectrometry Kobe University Graduate School of Medicine Kobe Japan

5. Department of Cardiovascular Medicine National Cerebral and Cardiovascular Center Osaka Japan

6. Faculty of Medicine Universitas Indonesia Jakarta Indonesia

7. Department of Materials Science and Engineering Meijo University Nagoya Japan

8. Department of Dermatology, Division of Medicine for Function and Morphology of Sensory Organs, Faculty of Medicine Osaka Medical and Pharmaceutical University, Takatsuki Osaka Japan

Abstract

Background Ultraviolet B (UV‐B) irradiation is an effective treatment for human cutaneous disorders and was shown to reduce experimental atherosclerosis by attenuating immunoinflammatory responses. The aim of this study was to clarify the effect of specific wavelengths of UV‐B on atherosclerosis and the underlying mechanisms focusing on immunoinflammatory responses. Methods and Results Based on light‐emitting diode technology, we developed novel devices that can emit 282 nm UV‐B, which we do not receive from natural sunlight, 301 nm UV‐B, and clinically available 312 nm UV‐B. We irradiated 6‐week‐old male atherosclerosis‐prone Apoe −/− (apolipoprotein E‐deficient) mice with specific wavelengths of UV‐B and evaluated atherosclerosis and immunoinflammatory responses by performing histological analysis, flow cytometry, biochemical assays, and liquid chromatography/mass spectrometry‐based lipidomics. Irradiation of 282 nm UV‐B but not 301 or 312 nm UV‐B significantly reduced the development of aortic root atherosclerotic plaques and plaque inflammation. This atheroprotection was associated with specifically augmented immune responses of anti‐inflammatory CD4 + Foxp3 (forkhead box P3) + regulatory T cells in lymphoid tissues, whereas responses of other immune cells were not substantially affected. Analysis of various lipid mediators revealed that 282 nm UV‐B markedly increased the ratio of proresolving to proinflammatory lipid mediators in the skin. Conclusions We demonstrated that 282 nm UV‐B irradiation effectively reduces aortic inflammation and the development of atherosclerosis by systemically augmenting regulatory T‐cell responses and modulating the balance between proresolving and proinflammatory lipid mediators in the skin. Our findings indicate that a novel 282 nm UV‐B phototherapy could be an attractive approach to treat atherosclerosis.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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