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Optical Control of Mammalian Endogenous Transcription and Epigenetic States

The dynamic nature of gene expression enables cellular programming, homeostasis, and environmental adaptation in living systems. Dissection of causal gene functions in cellular and organismal processes therefore necessitates approaches that enable spatially and temporally precise modulation of gene...

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Autores principales: Konermann, Silvana, Brigham, Mark D., Trevino, Alexandro, Hsu, Patrick D., Heidenreich, Matthias, Cong, Le, Platt, Randall J., Scott, David A., Church, George M., Zhang, Feng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3856241/
https://www.ncbi.nlm.nih.gov/pubmed/23877069
http://dx.doi.org/10.1038/nature12466
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author Konermann, Silvana
Brigham, Mark D.
Trevino, Alexandro
Hsu, Patrick D.
Heidenreich, Matthias
Cong, Le
Platt, Randall J.
Scott, David A.
Church, George M.
Zhang, Feng
author_facet Konermann, Silvana
Brigham, Mark D.
Trevino, Alexandro
Hsu, Patrick D.
Heidenreich, Matthias
Cong, Le
Platt, Randall J.
Scott, David A.
Church, George M.
Zhang, Feng
author_sort Konermann, Silvana
collection PubMed
description The dynamic nature of gene expression enables cellular programming, homeostasis, and environmental adaptation in living systems. Dissection of causal gene functions in cellular and organismal processes therefore necessitates approaches that enable spatially and temporally precise modulation of gene expression. Recently, a variety of microbial and plant-derived light-sensitive proteins have been engineered as optogenetic actuators, enabling high precision spatiotemporal control of many cellular functions(1-11). However, versatile and robust technologies that enable optical modulation of transcription in the mammalian endogenous genome remain elusive. Here, we describe the development of Light-Inducible Transcriptional Effectors (LITEs), an optogenetic two-hybrid system integrating the customizable TALE DNA-binding domain(12-14) with the light-sensitive cryptochrome 2 protein and its interacting partner CIB1 from Arabidopsis thaliana. LITEs do not require additional exogenous chemical co-factors, are easily customized to target many endogenous genomic loci, and can be activated within minutes with reversibility(3,4,6,7,15). LITEs can be packaged into viral vectors and genetically targeted to probe specific cell populations. We have applied this system in primary mouse neurons, as well as in the brain of awake mice in vivo to mediate reversible modulation of mammalian endogenous gene expression as well as targeted epigenetic chromatin modifications. The LITE system establishes a novel mode of optogenetic control of endogenous cellular processes and enables direct testing of the causal roles of genetic and epigenetic regulation in normal biological processes and disease states.
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spelling pubmed-38562412014-02-23 Optical Control of Mammalian Endogenous Transcription and Epigenetic States Konermann, Silvana Brigham, Mark D. Trevino, Alexandro Hsu, Patrick D. Heidenreich, Matthias Cong, Le Platt, Randall J. Scott, David A. Church, George M. Zhang, Feng Nature Article The dynamic nature of gene expression enables cellular programming, homeostasis, and environmental adaptation in living systems. Dissection of causal gene functions in cellular and organismal processes therefore necessitates approaches that enable spatially and temporally precise modulation of gene expression. Recently, a variety of microbial and plant-derived light-sensitive proteins have been engineered as optogenetic actuators, enabling high precision spatiotemporal control of many cellular functions(1-11). However, versatile and robust technologies that enable optical modulation of transcription in the mammalian endogenous genome remain elusive. Here, we describe the development of Light-Inducible Transcriptional Effectors (LITEs), an optogenetic two-hybrid system integrating the customizable TALE DNA-binding domain(12-14) with the light-sensitive cryptochrome 2 protein and its interacting partner CIB1 from Arabidopsis thaliana. LITEs do not require additional exogenous chemical co-factors, are easily customized to target many endogenous genomic loci, and can be activated within minutes with reversibility(3,4,6,7,15). LITEs can be packaged into viral vectors and genetically targeted to probe specific cell populations. We have applied this system in primary mouse neurons, as well as in the brain of awake mice in vivo to mediate reversible modulation of mammalian endogenous gene expression as well as targeted epigenetic chromatin modifications. The LITE system establishes a novel mode of optogenetic control of endogenous cellular processes and enables direct testing of the causal roles of genetic and epigenetic regulation in normal biological processes and disease states. 2013-08-23 2013-08-22 /pmc/articles/PMC3856241/ /pubmed/23877069 http://dx.doi.org/10.1038/nature12466 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Konermann, Silvana
Brigham, Mark D.
Trevino, Alexandro
Hsu, Patrick D.
Heidenreich, Matthias
Cong, Le
Platt, Randall J.
Scott, David A.
Church, George M.
Zhang, Feng
Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title_full Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title_fullStr Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title_full_unstemmed Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title_short Optical Control of Mammalian Endogenous Transcription and Epigenetic States
title_sort optical control of mammalian endogenous transcription and epigenetic states
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3856241/
https://www.ncbi.nlm.nih.gov/pubmed/23877069
http://dx.doi.org/10.1038/nature12466
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