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The simultaneous detection of mitochondrial DNA damage from sun-exposed skin of three whale species and its association with UV-induced microscopic lesions and apoptosis
Authors:Amy Bowman  Laura M. Martinez-Levasseur  Karina Acevedo-Whitehouse  Diane Gendron  Mark A. Birch-Machin
Affiliation:1. Dermatological Sciences, Institute of Cellular Medicine, Newcastle University, Newcastle upon Tyne NE2 4HH, UK;2. Institute of Zoology, Zoological Society of London, Regent''s Park, London NW1 4RY, UK;3. School of Biological and Chemical Sciences, Queen Mary University of London, Mile End Road, London E1 4NS, UK;4. Department of Biology, Trent University, 1600 West Bank Dr, Peterborough K9J 7B8, Canada;5. Unit for Basic and Applied Microbiology, School of Natural Sciences, Autonomous University of Queretaro, Mexico;6. Centro Interdisciplinario de Ciencias Marinas, Instituto Politécnico Nacional, s/n Col. Playa Palo de Santa Rita, La Paz, BCS 23096, Mexico
Abstract:Due to life history and physiological constraints, cetaceans (whales) are unable to avoid prolonged exposure to external environmental insults, such as solar ultraviolet radiation (UV). The majority of studies on the effects of UV on skin are restricted to humans and laboratory animals, but it is important to develop tools to understand the effects of UV damage on large mammals such as whales, as these animals are long-lived and widely distributed, and can reflect the effects of UV across a large geographical range. We and others have used mitochondrial DNA (mtDNA) as a reliable marker of UV-induced damage particularly in human skin. UV-induced mtDNA strand breaks or lesions accumulate throughout the lifespan of an individual, thus constituting an excellent biomarker for cumulative exposure. Based on our previous studies in human skin, we have developed for the first time in the literature a quantitative real-time PCR methodology to detect and quantify mtDNA lesions in skin from sun-blistered whales. Furthermore the methodology allows for simultaneous detection of mtDNA damage in different species. Therefore using 44 epidermal mtDNA samples collected from 15 blue whales, 10 fin whales, and 19 sperm whales from the Gulf of California, Mexico, we quantified damage across 4.3 kilobases, a large region of the ~ 16,400 base pair whale mitochondrial genome. The results show a range of mtDNA damage in the skin of the three different whale species. This previously unreported observation was correlated with apoptotic damage and microscopic lesions, both of which are markers of UV-induced damage. As is the case in human studies, this suggests the potential use of mtDNA as a biomarker for measuring the effect of cumulative UV exposure in whales and may provide a platform to help understand the effects of changing global environmental conditions.
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