Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells

Melanin protects the skin and eyes from the harmful effects of UV irradiation, protects neural cells from toxic insults, and is required for sound conduction in the inner ear. Aberrant regulation of melanogenesis underlies skin disorders (melasma and vitiligo), neurologic disorders (Parkinson's...

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Autores principales: Ganesan, Anand K., Ho, Hsiang, Bodemann, Brian, Petersen, Sean, Aruri, Jayavani, Koshy, Shiney, Richardson, Zachary, Le, Lu Q., Krasieva, Tatiana, Roth, Michael G., Farmer, Pat, White, Michael A.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2585813/
https://www.ncbi.nlm.nih.gov/pubmed/19057677
http://dx.doi.org/10.1371/journal.pgen.1000298
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author Ganesan, Anand K.
Ho, Hsiang
Bodemann, Brian
Petersen, Sean
Aruri, Jayavani
Koshy, Shiney
Richardson, Zachary
Le, Lu Q.
Krasieva, Tatiana
Roth, Michael G.
Farmer, Pat
White, Michael A.
author_facet Ganesan, Anand K.
Ho, Hsiang
Bodemann, Brian
Petersen, Sean
Aruri, Jayavani
Koshy, Shiney
Richardson, Zachary
Le, Lu Q.
Krasieva, Tatiana
Roth, Michael G.
Farmer, Pat
White, Michael A.
author_sort Ganesan, Anand K.
collection PubMed
description Melanin protects the skin and eyes from the harmful effects of UV irradiation, protects neural cells from toxic insults, and is required for sound conduction in the inner ear. Aberrant regulation of melanogenesis underlies skin disorders (melasma and vitiligo), neurologic disorders (Parkinson's disease), auditory disorders (Waardenburg's syndrome), and opthalmologic disorders (age related macular degeneration). Much of the core synthetic machinery driving melanin production has been identified; however, the spectrum of gene products participating in melanogenesis in different physiological niches is poorly understood. Functional genomics based on RNA-mediated interference (RNAi) provides the opportunity to derive unbiased comprehensive collections of pharmaceutically tractable single gene targets supporting melanin production. In this study, we have combined a high-throughput, cell-based, one-well/one-gene screening platform with a genome-wide arrayed synthetic library of chemically synthesized, small interfering RNAs to identify novel biological pathways that govern melanin biogenesis in human melanocytes. Ninety-two novel genes that support pigment production were identified with a low false discovery rate. Secondary validation and preliminary mechanistic studies identified a large panel of targets that converge on tyrosinase expression and stability. Small molecule inhibition of a family of gene products in this class was sufficient to impair chronic tyrosinase expression in pigmented melanoma cells and UV-induced tyrosinase expression in primary melanocytes. Isolation of molecular machinery known to support autophagosome biosynthesis from this screen, together with in vitro and in vivo validation, exposed a close functional relationship between melanogenesis and autophagy. In summary, these studies illustrate the power of RNAi-based functional genomics to identify novel genes, pathways, and pharmacologic agents that impact a biological phenotype and operate outside of preconceived mechanistic relationships.
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spelling pubmed-25858132008-12-05 Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells Ganesan, Anand K. Ho, Hsiang Bodemann, Brian Petersen, Sean Aruri, Jayavani Koshy, Shiney Richardson, Zachary Le, Lu Q. Krasieva, Tatiana Roth, Michael G. Farmer, Pat White, Michael A. PLoS Genet Research Article Melanin protects the skin and eyes from the harmful effects of UV irradiation, protects neural cells from toxic insults, and is required for sound conduction in the inner ear. Aberrant regulation of melanogenesis underlies skin disorders (melasma and vitiligo), neurologic disorders (Parkinson's disease), auditory disorders (Waardenburg's syndrome), and opthalmologic disorders (age related macular degeneration). Much of the core synthetic machinery driving melanin production has been identified; however, the spectrum of gene products participating in melanogenesis in different physiological niches is poorly understood. Functional genomics based on RNA-mediated interference (RNAi) provides the opportunity to derive unbiased comprehensive collections of pharmaceutically tractable single gene targets supporting melanin production. In this study, we have combined a high-throughput, cell-based, one-well/one-gene screening platform with a genome-wide arrayed synthetic library of chemically synthesized, small interfering RNAs to identify novel biological pathways that govern melanin biogenesis in human melanocytes. Ninety-two novel genes that support pigment production were identified with a low false discovery rate. Secondary validation and preliminary mechanistic studies identified a large panel of targets that converge on tyrosinase expression and stability. Small molecule inhibition of a family of gene products in this class was sufficient to impair chronic tyrosinase expression in pigmented melanoma cells and UV-induced tyrosinase expression in primary melanocytes. Isolation of molecular machinery known to support autophagosome biosynthesis from this screen, together with in vitro and in vivo validation, exposed a close functional relationship between melanogenesis and autophagy. In summary, these studies illustrate the power of RNAi-based functional genomics to identify novel genes, pathways, and pharmacologic agents that impact a biological phenotype and operate outside of preconceived mechanistic relationships. Public Library of Science 2008-12-05 /pmc/articles/PMC2585813/ /pubmed/19057677 http://dx.doi.org/10.1371/journal.pgen.1000298 Text en Ganesan et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ganesan, Anand K.
Ho, Hsiang
Bodemann, Brian
Petersen, Sean
Aruri, Jayavani
Koshy, Shiney
Richardson, Zachary
Le, Lu Q.
Krasieva, Tatiana
Roth, Michael G.
Farmer, Pat
White, Michael A.
Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title_full Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title_fullStr Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title_full_unstemmed Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title_short Genome-Wide siRNA-Based Functional Genomics of Pigmentation Identifies Novel Genes and Pathways That Impact Melanogenesis in Human Cells
title_sort genome-wide sirna-based functional genomics of pigmentation identifies novel genes and pathways that impact melanogenesis in human cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2585813/
https://www.ncbi.nlm.nih.gov/pubmed/19057677
http://dx.doi.org/10.1371/journal.pgen.1000298
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