Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy

Potent melanin production enhancement of human tyrosinase plasmid (pAH7/Tyr, P) in mouse melanoma cells (B 16F 10) by Tat peptide (T) and an entrapment in elastic cationic niosomes (E) was described. The E composed of Tween 61/cholesterol/dodecyl dimethyl ammonium bromide at 1:1:0.5 molar ratio was...

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Main Authors: Manosroi J., Khositsuntiwong N., Gotz F., Werner R.G., Manosroi W., Manosroi A.
Format: Article
Language:English
Published: 2014
Online Access:http://www.scopus.com/inward/record.url?eid=2-s2.0-84868106277&partnerID=40&md5=10d546917cc9ec68c7117dd852581de1
http://cmuir.cmu.ac.th/handle/6653943832/3944
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spelling th-cmuir.6653943832-39442014-08-30T02:35:30Z Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy Manosroi J. Khositsuntiwong N. Gotz F. Werner R.G. Manosroi W. Manosroi A. Potent melanin production enhancement of human tyrosinase plasmid (pAH7/Tyr, P) in mouse melanoma cells (B 16F 10) by Tat peptide (T) and an entrapment in elastic cationic niosomes (E) was described. The E composed of Tween 61/cholesterol/dodecyl dimethyl ammonium bromide at 1:1:0.5 molar ratio was prepared by freeze-dried emptying liposomes method. PE at P/E ratio of 1:160 w/w and TPE at T/P/E ratio of 0.125:1:160, 0.25:1:160, and 0.5:1:160 w/w/w were prepared. The final concentration of the plasmid in the study was 4ng/μL. By sulforhodamine B assay, PE and TPE complexes showed slight or no cytotoxic effect. The cells transfected with TPE (0.5:1:160) exhibited the highest enhancement of tyrosinase enzyme activity of 11.82-, 7.67-, 5.07-, and 6.29-folds of control, P, PE, and TP (0.5:1) and melanin production of 13.03-, 8.46-, 5.36-, and 6.58-folds of control, P, PE, and TP (0.5:1), respectively. The elastic cationic niosomes demonstrated an increase in thermal stability of P at 4±2, 25±2, and 45±2°C. The vesicular size and the zeta potential values of PE and TPE complexes were slightly increased but still in the range of stable dispersion (out of ±30mV). These results indicated the high potential application of the TPE complexes for further investigation for vitiligo gene therapy. TPE complexes exhibited potent enhancement of tryosinase gene expression and melanin production in melanoma cell line (B 16F 10). This result indicated the high potential application of the TPE complexes for further investigation for vitiligo gene theraphy. © 2012 John Wiley & Sons A/S. 2014-08-30T02:35:30Z 2014-08-30T02:35:30Z 2012 Article 17470277 10.1111/cbdd.12048 CBDDA http://www.scopus.com/inward/record.url?eid=2-s2.0-84868106277&partnerID=40&md5=10d546917cc9ec68c7117dd852581de1 http://cmuir.cmu.ac.th/handle/6653943832/3944 English
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
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language English
description Potent melanin production enhancement of human tyrosinase plasmid (pAH7/Tyr, P) in mouse melanoma cells (B 16F 10) by Tat peptide (T) and an entrapment in elastic cationic niosomes (E) was described. The E composed of Tween 61/cholesterol/dodecyl dimethyl ammonium bromide at 1:1:0.5 molar ratio was prepared by freeze-dried emptying liposomes method. PE at P/E ratio of 1:160 w/w and TPE at T/P/E ratio of 0.125:1:160, 0.25:1:160, and 0.5:1:160 w/w/w were prepared. The final concentration of the plasmid in the study was 4ng/μL. By sulforhodamine B assay, PE and TPE complexes showed slight or no cytotoxic effect. The cells transfected with TPE (0.5:1:160) exhibited the highest enhancement of tyrosinase enzyme activity of 11.82-, 7.67-, 5.07-, and 6.29-folds of control, P, PE, and TP (0.5:1) and melanin production of 13.03-, 8.46-, 5.36-, and 6.58-folds of control, P, PE, and TP (0.5:1), respectively. The elastic cationic niosomes demonstrated an increase in thermal stability of P at 4±2, 25±2, and 45±2°C. The vesicular size and the zeta potential values of PE and TPE complexes were slightly increased but still in the range of stable dispersion (out of ±30mV). These results indicated the high potential application of the TPE complexes for further investigation for vitiligo gene therapy. TPE complexes exhibited potent enhancement of tryosinase gene expression and melanin production in melanoma cell line (B 16F 10). This result indicated the high potential application of the TPE complexes for further investigation for vitiligo gene theraphy. © 2012 John Wiley & Sons A/S.
format Article
author Manosroi J.
Khositsuntiwong N.
Gotz F.
Werner R.G.
Manosroi W.
Manosroi A.
spellingShingle Manosroi J.
Khositsuntiwong N.
Gotz F.
Werner R.G.
Manosroi W.
Manosroi A.
Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
author_facet Manosroi J.
Khositsuntiwong N.
Gotz F.
Werner R.G.
Manosroi W.
Manosroi A.
author_sort Manosroi J.
title Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
title_short Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
title_full Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
title_fullStr Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
title_full_unstemmed Potent Melanin Production Enhancement of Human Tyrosinase Gene by Tat and an Entrapment in Elastic Cationic Niosomes: Potential Application in Vitiligo Gene Therapy
title_sort potent melanin production enhancement of human tyrosinase gene by tat and an entrapment in elastic cationic niosomes: potential application in vitiligo gene therapy
publishDate 2014
url http://www.scopus.com/inward/record.url?eid=2-s2.0-84868106277&partnerID=40&md5=10d546917cc9ec68c7117dd852581de1
http://cmuir.cmu.ac.th/handle/6653943832/3944
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