The generation of reactive oxygen species has been implicated as part of the mechanism responsible for UVB-radiation-induced skin damage. In mice, evidence suggests that increased dietary selenium intake may protect skin from many of the harmful effects of UVB radiation. We sought to determine the selenoprotein profile of cultured human skin cells and whether selenium supplementation could protect keratinocytes and melanocytes from the lethal effects of UVB radiation. Labelling experiments using [75Se]selenite showed qualitative and quantitative differences in selenoprotein expression by human fibroblasts, keratinocytes and melanocytes. This was most noticeable for thioredoxin reductase (60 kDa) and phospholipid glutathione peroxidase (21 kDa); these proteins were identified by Western blotting. Despite these differences, we found that a 24 h preincubation with sodium selenite or selenomethionine protected both cultured human keratinocytes and melanocytes from UVB-induced cell death. With primary keratinocytes, the greatest reduction in cell death was found with 10 nM sodium selenite (79% cell death reduced to 21.7%; P< 0.01) and with 50 nM selenomethionine (79% cell death reduced to 13.2%; P< 0.01). Protection could be obtained with concentrations as low as 1 nM with sodium selenite and 10 nM with selenomethionine. When selenium was added after UVB radiation, little protection could be achieved, with cell death only being reduced from 88.5% to about 50% with both compounds. In all of the experiments sodium selenite was more potent than selenomethionine at providing protection from UVB radiation.
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May 1998
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Research Article|
May 15 1998
Differential expression of selenoproteins by human skin cells and protection by selenium from UVB-radiation-induced cell death Available to Purchase
Teresa S. RAFFERTY;
Teresa S. RAFFERTY
1
*Department of Dermatology, University of Edinburgh, Lauriston Place, Edinburgh EH3 9YW, Scotland, U.K.
1To whom correspondence should be addressed (e-mail [email protected]).
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Roderick C. McKENZIE;
Roderick C. McKENZIE
*Department of Dermatology, University of Edinburgh, Lauriston Place, Edinburgh EH3 9YW, Scotland, U.K.
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John A. A. HUNTER;
John A. A. HUNTER
*Department of Dermatology, University of Edinburgh, Lauriston Place, Edinburgh EH3 9YW, Scotland, U.K.
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A. Forbes HOWIE;
A. Forbes HOWIE
†Department of Clinical Biochemistry, University of Edinburgh, Lauriston Place, Edinburgh EH3 9YW, Scotland, U.K.
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John R. ARTHUR;
John R. ARTHUR
‡Rowett Research Institute, Bucksburn, Aberdeen AB21 9SB, Scotland, U.K.
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Fergus NICOL;
Fergus NICOL
‡Rowett Research Institute, Bucksburn, Aberdeen AB21 9SB, Scotland, U.K.
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Geoff J. BECKETT
Geoff J. BECKETT
†Department of Clinical Biochemistry, University of Edinburgh, Lauriston Place, Edinburgh EH3 9YW, Scotland, U.K.
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Publisher: Portland Press Ltd
Received:
January 05 1998
Revision Received:
February 06 1998
Accepted:
February 24 1998
Online ISSN: 1470-8728
Print ISSN: 0264-6021
The Biochemical Society, London © 1998
1998
Biochem J (1998) 332 (1): 231–236.
Article history
Received:
January 05 1998
Revision Received:
February 06 1998
Accepted:
February 24 1998
Citation
Teresa S. RAFFERTY, Roderick C. McKENZIE, John A. A. HUNTER, A. Forbes HOWIE, John R. ARTHUR, Fergus NICOL, Geoff J. BECKETT; Differential expression of selenoproteins by human skin cells and protection by selenium from UVB-radiation-induced cell death. Biochem J 15 May 1998; 332 (1): 231–236. doi: https://doi.org/10.1042/bj3320231
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