Literature DB >> 27667312

Oxidative stress and ageing.

M A Birch-Machin1, A Bowman2.   

Abstract

Oxidative stress is the resultant damage due to redox imbalances (increase in destructive free radicals [reactive oxygen species (ROS)] and reduction in antioxidant protection/pathways) and is linked to ageing in many tissues including skin. In ageing skin there are bioenergetic differences between keratinocytes and fibroblasts which provide a potential ageing biomarker. The differences in skin bioenergy are part of the mitochondrial theory of ageing which remains one of the most widely accepted ageing theories describing subsequent increasing free radical generation. Mitochondria are the major source of cellular oxidative stress and form part of the vicious cycle theory of ageing. External and internal sources of oxidative stress include UVR/IR, pollution (environment), lifestyle (exercise and diet), alcohol and smoking all of which may potentially impact on skin although many exogenous actives and endogenous antioxidant defence systems have been described to help abrogate the increased stress. This also links to differences in skin cell types in terms of the UVR action spectrum for nuclear and mitochondrial DNA damage (the latter a previously described UVR biomarker in skin). Recent work associates bioenergy production and oxidative stress with pigment production thereby providing another additional potential avenue for targeted anti-ageing intervention in skin. This new data supporting the detrimental effects of the numerous wavelengths of UVR may aid in the development of cosmetic/sunscreen design to reduce the effects of photoageing. Recently, complex II of the mitochondrial electron transport chain appears to be more important than previously thought in the generation of free radicals (suggested predominantly by non-human studies). We investigated the relationship between complex II and ageing using human skin as a model tissue. The rate of complex II activity per unit of mitochondria was determined in fibroblasts and keratinocytes cultured from skin covering a wide age range. Complex II activity significantly decreased with age in fibroblasts (P = 0·015), but not in keratinocytes. This was associated with a significant decline in transcript expression (P = 0·008 and P = 0·001) and protein levels (P = 0·0006 and P = 0·005) of the SDHA and SDHB catalytic subunits of complex II respectively. In addition there was a significant decrease in complex II activity with age (P = 0·029) that was specific to senescent skin cells, our study being the first to investigate these differences with senescence and skin age. There was no decrease in complex IV activity with increasing age, suggesting possible locality to complex II. Our study provides a future potential biomarker for monitoring the progression of skin ageing.
© 2016 British Association of Dermatologists.

Entities:  

Year:  2016        PMID: 27667312     DOI: 10.1111/bjd.14906

Source DB:  PubMed          Journal:  Br J Dermatol        ISSN: 0007-0963            Impact factor:   9.302


  26 in total

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6.  Biomarkers of nucleic acid oxidation - A summary state-of-the-art.

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9.  A novel role for NUPR1 in the keratinocyte stress response to UV oxidized phospholipids.

Authors:  Marie-Sophie Narzt; Ionela-Mariana Nagelreiter; Olga Oskolkova; Valery N Bochkov; Julie Latreille; Maria Fedorova; Zhixu Ni; Fernando J Sialana; Gert Lubec; Manuel Filzwieser; Maria Laggner; Martin Bilban; Michael Mildner; Erwin Tschachler; Johannes Grillari; Florian Gruber
Journal:  Redox Biol       Date:  2018-11-13       Impact factor: 11.799

10.  Next-Generation Sequencing and Quantitative Proteomics of Hutchinson-Gilford progeria syndrome-derived cells point to a role of nucleotide metabolism in premature aging.

Authors:  Jesús Mateos; Juan Fafián-Labora; Miriam Morente-López; Iván Lesende-Rodriguez; Lorenzo Monserrat; María A Ódena; Eliandre de Oliveira; Javier de Toro; María C Arufe
Journal:  PLoS One       Date:  2018-10-31       Impact factor: 3.240

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