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Impact of hyperpigmentation on superoxide flux and melanoma cell metabolism at mitochondrial complex II. | LitMetric

Impact of hyperpigmentation on superoxide flux and melanoma cell metabolism at mitochondrial complex II.

FASEB J

Dermatological Sciences, Institute of Cellular Medicine, Medical School, Newcastle University, Newcastle upon Tyne, United Kingdom

Published: January 2015

AI Article Synopsis

  • - Melanogenesis is a natural process that helps protect cells from UV damage, but the links between mitochondrial function and skin pigmentation haven't been fully understood.
  • - Research showed a strong correlation between cell pigmentation and the activity of complex II in mitochondria across various melanoma cell lines, indicating that more pigmentation is tied to increased mitochondrial function.
  • - The study reveals that increased pigmentation also correlates with higher superoxide production at complex II, suggesting that hyperpigmentation might serve as a protective antioxidant response against reactive oxygen species generated through mitochondrial activity.

Article Abstract

Melanogenesis is a highly conserved process of cytophotoprotection from UV radiation present in many species. Although both mitochondrial function and UV radiation insults are well-documented promoters of increased cellular stress, their individual molecular relationships with skin pigmentation have not been clearly resolved. This study provides evidence for a direct relationship between cellular melanin content, superoxide flux, and mitochondrial function at complex II. Direct and significant correlation between increased pigmentation and complex II turnover was observed in genetically different melanoma cell lines of varied basal pigmentation states (P < 0.01). The same trend was also observed when comparing genetically identical cell cultures with increasing levels of induced pigmentation (P < 0.005). The observation of increased steady-state levels of the catalytic complex II succinate dehydrogenase subunit A alongside hyperpigmentation suggested coregulation of activity and pigment production (P < 0.01). The study also presents novel evidence for a relationship between hyperpigmentation and increased superoxide-generating capacity at complex II. By amperometrically monitoring superoxide flux from differently pigmented FM55 melanocytes and their isolated mitochondria, a dynamic and responsive relationship between pigmentation, complex II function, and intracellular superoxide generation was observed (P < 0.005). The data support hyperpigmentation as a protective antioxidant mechanism in response to complex II-mediated reactive oxygen species generation.

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Source
http://dx.doi.org/10.1096/fj.14-261982DOI Listing

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