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Post-translational processing of melanogenesis subsequent to melanogenic protein expression and its regulation leading to the development of novel depigmenting agents
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- 한국생물공학회 바로가기
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- 간행물
- 한국생물공학회 학술대회 바로가기
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- 통권
- 2008 추계학술대회 및 국제심포지움 (2008.10)바로가기
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- 페이지
- pp.5-5
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- 저자
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- 언어
- 영어(ENG)
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- URL
- https://www.earticle.net/Article/A99040
※ 원문제공기관과의 협약기간이 종료되어 열람이 제한될 수 있습니다.
원문정보
초록
- 영어
- Hyperpigmentation mechanisms including UVB-melanosis have been recently progressed in terms of paracrine cytokine regulation between melanocytes and keratinocytes/fibroblasts as well as of endothelins or stem cell factor-induced intracellular signalings leading to gene expression of melanogenic molecules including tyrosinase, endothelin B receptor or melanosomal protein Pmel17. According to these mechanisms, several novel depigmenting agents have recently been developed. However, post-translational processing of
melanogenesis subsequent to gene and protein expression of melanogenic molecules including tyrosinase and Pmel 17 is poorly understood and there is few depigmenting agents developed based on the above strategy.
Previously we found that the recovery process of melanization following glycosylation inhibition of B-16 melanoma cells which induces complete loss of melanization in melanosome due to the interrupted transfer of tyrosinases compartmentalized in coated vesicles is a good tool for searching post-translational regulation of melanogenesis. In this study, using the pigmentation recovery process of glycosylation-inhibited B-16 melanoma cells and western blotting analysis, we determined whether tyrosinases are originally present in immature melanosome or is transferred from Golgi area to melanosomes. In glycosylation-inhibited B-16 melanoma cells, tyrosinases are not localized in melanosome-rich fraction but in cytosol fraction, indicating
that tyrosinases are transferred from Gogi area to melanosomes. The addition of reduced glutathione into the recovery process abolished the recovered translocation of tyrosinases from Gogi-endoplasmic reticulum-lysosome(GERL) to melanosomes despite no glycosylation inhibition potential of reduced glutathione, resulting in the continuous complete loss of melanization. These findings suggest that reduced glutathione serves as a translocation inhibitor for tyrosinases but not as a tyrosinase inhibitor. To assess whether glycosylation inhibitors have a potential to inhibit epidermal hyperpigmentation stimulated by melanogenic cytokines released from UVB-exposed keratinocytes, we used guinea pig skin organ culture or three-dimensional cultures consisting of human keratinocytes and human melanocytes to examine the inhibitory effect of glycosylation inhibitors on epidermal pigmentation. In both models, glycosylation
inhibitors markedly abolished visibly increased pigmentation without affecting increased melanocyte population. The present study suggests that glycosylation inhibitors or reduced gluthathione can serve as novel depigmenting agents with unique strategy such as intracellular translocation inhibition if they can penetrate into the epidermis at effective concentrations when topically applied.
저자
간행물 정보
발행기관
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- 발행기관명
- 한국생물공학회 [The Korean Society for Biotechnology and Bioengineering]
- 설립연도
- 1984
- 분야
- 공학>생물공학
- 소개
- 이 법인은 생물 공학의 발전과 보급에 이바지하고, 회원 상호 간의 연구 협력과 친목을 도모함을 목적으로 한다 1. 생물공학 분야의 발전을 위한 연구 협력 2. 생물공학의 실용화를 촉진시키기 위한 산학 협동 3. 학술연구 발표회, 강연회, 연수회 등 학술활동의 개최 4. 국,영문 학술지,소식지,학술회의 Proceedings 및 학술도서의 발간 5. 생물공학 발전을 위한 정책 건의 6. 기타 국제 교류 등 본 학회의 목적 달성을 위한 제반 활동
간행물
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- 간행물명
- 한국생물공학회 학술대회
- 간기
- 반년간
- 수록기간
- 1985~2013
- 십진분류
- KDC 476 DDC 576
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