The antiwrinkle effect of topical concentrated 2‐dimethylaminoethanol involves a vacuolar cytopathology
Identifieur interne : 001A92 ( Main/Exploration ); précédent : 001A91; suivant : 001A93The antiwrinkle effect of topical concentrated 2‐dimethylaminoethanol involves a vacuolar cytopathology
Auteurs : G. Morissette [Canada] ; L. Germain [Canada] ; F. Marceau [Canada]Source :
- British Journal of Dermatology [ 0007-0963 ] ; 2007-03.
English descriptors
- Teeft :
- Amine, Amine drugs, Antiwrinkle effect, Apparent skin fullness, Arrowheads point, Authors journal compilation, British association, Broblasts, Cell death, Cell washout, Cells pretreated, Certain depth, Complete culture medium, Cultured cells, Cultured rabbit, Cutaneous, Cytopathology, Cytotoxicity, Cytotoxicity assay, Dermatologist, Dermatologists british journal, Dermatology, Dimethyl sulphoxide, Dmae, Dmae mmol, Dmae reservoir, Emla cream, Epidermal, Epidermal cells, Epidermal thickness, Epidermis, Fresh culture medium, Higher concentration level, Human cutaneous epithelial cells, Human epidermal cells, Inner skin, Koilocytic cells, Local anaesthetics, Massive cell vacuolization, Massive vacuolization, Millimolar drug concentration, Mitotic, Mitotic arrest, Mmol, Mmol concentration, Morissette, Morphological effect, Morphological response, Nonviable cells, Organic amines, Other amines, Petri dishes, Phase contrast, Phase contrast observations, Photographic record, Ploidy, Primary cultures, Procainamide, Propidium iodide, Rapid effect, Regular culture medium, Skin layers, Smooth muscle cells, Systemic absorption, Tertiary amine, Topical dmae, Triethanolamine, Vacuolar, Vacuolar adenosine triphosphatase, Vacuolar cell expansion, Vacuolar cytopathology, Vacuolization, Vacuolization response, Various sizes, Various time periods.
Abstract
Background The ‘cosmeceutical’ agent 2‐dimethylaminoethanol (DMAE) is a tertiary amine found in high concentration in numerous topical antiwrinkle preparations. Objectives We hypothesized that a 337 mmol L−1 (3%) DMAE reservoir applied to the skin could reproduce the cytopathology induced by other amines by maintaining a millimolar drug concentration within a certain depth of the skin layers, and that vacuolar cell expansion could account for the very rapid effect on the apparent skin fullness. Methods Morphological and functional assays were applied to cultured rabbit dermal fibroblasts treated with tertiary amines in vitro. A morphological verification of the vacuolization caused by topical DMAE was also attempted in vivo using the inner skin of the rabbit ear and in vitro using primary cultures of human cutaneous epithelial cells. Results Fibroblasts responded to DMAE (2·5–10 mmol L−1) by massive vacuolization (0·5–4 h; phase contrast observations). Triethanolamine, another chemical frequently used topically, was also active in this respect (10 mmol L−1). The vacuolar adenosine triphosphatase inhibitor bafilomycin A1 prevented DMAE‐ or triethanolamine‐induced vacuolization; adding bafilomycin A1 or cell washout slowly reversed the established vacuolization induced by DMAE. Further effects of DMAE in cultured fibroblasts included a moderate cytotoxicity (10 mmol L−1) that was abated by bafilomycin A1 cotreatment, a concentration‐dependent mitotic arrest (2·5 mmol L−1) and transient and mild effects on cell ploidy. The epidermis of the rabbit external ear was significantly thickened and exhibited clear perinuclear swelling indicative of vacuolization in response to 3% DMAE (1 h; paraffin tissue sections). Cultured human cutaneous epithelial cells responded to DMAE by vacuolization (inhibited by bafilomycin A1 cotreatment). Conclusions The vacuolar cytopathology induced by concentrated organic amines may be the cellular basis of the antiwrinkle effect of DMAE.
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DOI: 10.1111/j.1365-2133.2007.07681.x
Affiliations:
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Objectives We hypothesized that a 337 mmol L−1 (3%) DMAE reservoir applied to the skin could reproduce the cytopathology induced by other amines by maintaining a millimolar drug concentration within a certain depth of the skin layers, and that vacuolar cell expansion could account for the very rapid effect on the apparent skin fullness. Methods Morphological and functional assays were applied to cultured rabbit dermal fibroblasts treated with tertiary amines in vitro. A morphological verification of the vacuolization caused by topical DMAE was also attempted in vivo using the inner skin of the rabbit ear and in vitro using primary cultures of human cutaneous epithelial cells. Results Fibroblasts responded to DMAE (2·5–10 mmol L−1) by massive vacuolization (0·5–4 h; phase contrast observations). Triethanolamine, another chemical frequently used topically, was also active in this respect (10 mmol L−1). The vacuolar adenosine triphosphatase inhibitor bafilomycin A1 prevented DMAE‐ or triethanolamine‐induced vacuolization; adding bafilomycin A1 or cell washout slowly reversed the established vacuolization induced by DMAE. Further effects of DMAE in cultured fibroblasts included a moderate cytotoxicity (10 mmol L−1) that was abated by bafilomycin A1 cotreatment, a concentration‐dependent mitotic arrest (2·5 mmol L−1) and transient and mild effects on cell ploidy. The epidermis of the rabbit external ear was significantly thickened and exhibited clear perinuclear swelling indicative of vacuolization in response to 3% DMAE (1 h; paraffin tissue sections). Cultured human cutaneous epithelial cells responded to DMAE by vacuolization (inhibited by bafilomycin A1 cotreatment). Conclusions The vacuolar cytopathology induced by concentrated organic amines may be the cellular basis of the antiwrinkle effect of DMAE.</div></front></TEI><affiliations><list><country><li>Canada</li></country></list><tree><country name="Canada"><noRegion><name sortKey="Morissette, G" sort="Morissette, G" uniqKey="Morissette G" first="G." last="Morissette">G. Morissette</name></noRegion><name sortKey="Germain, L" sort="Germain, L" uniqKey="Germain L" first="L." last="Germain">L. Germain</name><name sortKey="Marceau, F" sort="Marceau, F" uniqKey="Marceau F" first="F." last="Marceau">F. Marceau</name></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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