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An integrative ENCODE resource for cancer genomics

ENCODE comprises thousands of functional genomics datasets, and the encyclopedia covers hundreds of cell types, providing a universal annotation for genome interpretation. However, for particular applications, it may be advantageous to use a customized annotation. Here, we develop such a custom anno...

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Autores principales: Zhang, Jing, Lee, Donghoon, Dhiman, Vineet, Jiang, Peng, Xu, Jie, McGillivray, Patrick, Yang, Hongbo, Liu, Jason, Meyerson, William, Clarke, Declan, Gu, Mengting, Li, Shantao, Lou, Shaoke, Xu, Jinrui, Lochovsky, Lucas, Ung, Matthew, Ma, Lijia, Yu, Shan, Cao, Qin, Harmanci, Arif, Yan, Koon-Kiu, Sethi, Anurag, Gürsoy, Gamze, Schoenberg, Michael Rutenberg, Rozowsky, Joel, Warrell, Jonathan, Emani, Prashant, Yang, Yucheng T., Galeev, Timur, Kong, Xiangmeng, Liu, Shuang, Li, Xiaotong, Krishnan, Jayanth, Feng, Yanlin, Rivera-Mulia, Juan Carlos, Adrian, Jessica, Broach, James R, Bolt, Michael, Moran, Jennifer, Fitzgerald, Dominic, Dileep, Vishnu, Liu, Tingting, Mei, Shenglin, Sasaki, Takayo, Trevilla-Garcia, Claudia, Wang, Su, Wang, Yanli, Zang, Chongzhi, Wang, Daifeng, Klein, Robert J., Snyder, Michael, Gilbert, David M., Yip, Kevin, Cheng, Chao, Yue, Feng, Liu, X. Shirley, White, Kevin P., Gerstein, Mark
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7391744/
https://www.ncbi.nlm.nih.gov/pubmed/32728046
http://dx.doi.org/10.1038/s41467-020-14743-w
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author Zhang, Jing
Lee, Donghoon
Dhiman, Vineet
Jiang, Peng
Xu, Jie
McGillivray, Patrick
Yang, Hongbo
Liu, Jason
Meyerson, William
Clarke, Declan
Gu, Mengting
Li, Shantao
Lou, Shaoke
Xu, Jinrui
Lochovsky, Lucas
Ung, Matthew
Ma, Lijia
Yu, Shan
Cao, Qin
Harmanci, Arif
Yan, Koon-Kiu
Sethi, Anurag
Gürsoy, Gamze
Schoenberg, Michael Rutenberg
Rozowsky, Joel
Warrell, Jonathan
Emani, Prashant
Yang, Yucheng T.
Galeev, Timur
Kong, Xiangmeng
Liu, Shuang
Li, Xiaotong
Krishnan, Jayanth
Feng, Yanlin
Rivera-Mulia, Juan Carlos
Adrian, Jessica
Broach, James R
Bolt, Michael
Moran, Jennifer
Fitzgerald, Dominic
Dileep, Vishnu
Liu, Tingting
Mei, Shenglin
Sasaki, Takayo
Trevilla-Garcia, Claudia
Wang, Su
Wang, Yanli
Zang, Chongzhi
Wang, Daifeng
Klein, Robert J.
Snyder, Michael
Gilbert, David M.
Yip, Kevin
Cheng, Chao
Yue, Feng
Liu, X. Shirley
White, Kevin P.
Gerstein, Mark
author_facet Zhang, Jing
Lee, Donghoon
Dhiman, Vineet
Jiang, Peng
Xu, Jie
McGillivray, Patrick
Yang, Hongbo
Liu, Jason
Meyerson, William
Clarke, Declan
Gu, Mengting
Li, Shantao
Lou, Shaoke
Xu, Jinrui
Lochovsky, Lucas
Ung, Matthew
Ma, Lijia
Yu, Shan
Cao, Qin
Harmanci, Arif
Yan, Koon-Kiu
Sethi, Anurag
Gürsoy, Gamze
Schoenberg, Michael Rutenberg
Rozowsky, Joel
Warrell, Jonathan
Emani, Prashant
Yang, Yucheng T.
Galeev, Timur
Kong, Xiangmeng
Liu, Shuang
Li, Xiaotong
Krishnan, Jayanth
Feng, Yanlin
Rivera-Mulia, Juan Carlos
Adrian, Jessica
Broach, James R
Bolt, Michael
Moran, Jennifer
Fitzgerald, Dominic
Dileep, Vishnu
Liu, Tingting
Mei, Shenglin
Sasaki, Takayo
Trevilla-Garcia, Claudia
Wang, Su
Wang, Yanli
Zang, Chongzhi
Wang, Daifeng
Klein, Robert J.
Snyder, Michael
Gilbert, David M.
Yip, Kevin
Cheng, Chao
Yue, Feng
Liu, X. Shirley
White, Kevin P.
Gerstein, Mark
author_sort Zhang, Jing
collection PubMed
description ENCODE comprises thousands of functional genomics datasets, and the encyclopedia covers hundreds of cell types, providing a universal annotation for genome interpretation. However, for particular applications, it may be advantageous to use a customized annotation. Here, we develop such a custom annotation by leveraging advanced assays, such as eCLIP, Hi-C, and whole-genome STARR-seq on a number of data-rich ENCODE cell types. A key aspect of this annotation is comprehensive and experimentally derived networks of both transcription factors and RNA-binding proteins (TFs and RBPs). Cancer, a disease of system-wide dysregulation, is an ideal application for such a network-based annotation. Specifically, for cancer-associated cell types, we put regulators into hierarchies and measure their network change (rewiring) during oncogenesis. We also extensively survey TF-RBP crosstalk, highlighting how SUB1, a previously uncharacterized RBP, drives aberrant tumor expression and amplifies the effect of MYC, a well-known oncogenic TF. Furthermore, we show how our annotation allows us to place oncogenic transformations in the context of a broad cell space; here, many normal-to-tumor transitions move towards a stem-like state, while oncogene knockdowns show an opposing trend. Finally, we organize the resource into a coherent workflow to prioritize key elements and variants, in addition to regulators. We showcase the application of this prioritization to somatic burdening, cancer differential expression and GWAS. Targeted validations of the prioritized regulators, elements and variants using siRNA knockdowns, CRISPR-based editing, and luciferase assays demonstrate the value of the ENCODE resource.
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spelling pubmed-73917442020-08-12 An integrative ENCODE resource for cancer genomics Zhang, Jing Lee, Donghoon Dhiman, Vineet Jiang, Peng Xu, Jie McGillivray, Patrick Yang, Hongbo Liu, Jason Meyerson, William Clarke, Declan Gu, Mengting Li, Shantao Lou, Shaoke Xu, Jinrui Lochovsky, Lucas Ung, Matthew Ma, Lijia Yu, Shan Cao, Qin Harmanci, Arif Yan, Koon-Kiu Sethi, Anurag Gürsoy, Gamze Schoenberg, Michael Rutenberg Rozowsky, Joel Warrell, Jonathan Emani, Prashant Yang, Yucheng T. Galeev, Timur Kong, Xiangmeng Liu, Shuang Li, Xiaotong Krishnan, Jayanth Feng, Yanlin Rivera-Mulia, Juan Carlos Adrian, Jessica Broach, James R Bolt, Michael Moran, Jennifer Fitzgerald, Dominic Dileep, Vishnu Liu, Tingting Mei, Shenglin Sasaki, Takayo Trevilla-Garcia, Claudia Wang, Su Wang, Yanli Zang, Chongzhi Wang, Daifeng Klein, Robert J. Snyder, Michael Gilbert, David M. Yip, Kevin Cheng, Chao Yue, Feng Liu, X. Shirley White, Kevin P. Gerstein, Mark Nat Commun Article ENCODE comprises thousands of functional genomics datasets, and the encyclopedia covers hundreds of cell types, providing a universal annotation for genome interpretation. However, for particular applications, it may be advantageous to use a customized annotation. Here, we develop such a custom annotation by leveraging advanced assays, such as eCLIP, Hi-C, and whole-genome STARR-seq on a number of data-rich ENCODE cell types. A key aspect of this annotation is comprehensive and experimentally derived networks of both transcription factors and RNA-binding proteins (TFs and RBPs). Cancer, a disease of system-wide dysregulation, is an ideal application for such a network-based annotation. Specifically, for cancer-associated cell types, we put regulators into hierarchies and measure their network change (rewiring) during oncogenesis. We also extensively survey TF-RBP crosstalk, highlighting how SUB1, a previously uncharacterized RBP, drives aberrant tumor expression and amplifies the effect of MYC, a well-known oncogenic TF. Furthermore, we show how our annotation allows us to place oncogenic transformations in the context of a broad cell space; here, many normal-to-tumor transitions move towards a stem-like state, while oncogene knockdowns show an opposing trend. Finally, we organize the resource into a coherent workflow to prioritize key elements and variants, in addition to regulators. We showcase the application of this prioritization to somatic burdening, cancer differential expression and GWAS. Targeted validations of the prioritized regulators, elements and variants using siRNA knockdowns, CRISPR-based editing, and luciferase assays demonstrate the value of the ENCODE resource. Nature Publishing Group UK 2020-07-29 /pmc/articles/PMC7391744/ /pubmed/32728046 http://dx.doi.org/10.1038/s41467-020-14743-w Text en © The Author(s) 2020 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Zhang, Jing
Lee, Donghoon
Dhiman, Vineet
Jiang, Peng
Xu, Jie
McGillivray, Patrick
Yang, Hongbo
Liu, Jason
Meyerson, William
Clarke, Declan
Gu, Mengting
Li, Shantao
Lou, Shaoke
Xu, Jinrui
Lochovsky, Lucas
Ung, Matthew
Ma, Lijia
Yu, Shan
Cao, Qin
Harmanci, Arif
Yan, Koon-Kiu
Sethi, Anurag
Gürsoy, Gamze
Schoenberg, Michael Rutenberg
Rozowsky, Joel
Warrell, Jonathan
Emani, Prashant
Yang, Yucheng T.
Galeev, Timur
Kong, Xiangmeng
Liu, Shuang
Li, Xiaotong
Krishnan, Jayanth
Feng, Yanlin
Rivera-Mulia, Juan Carlos
Adrian, Jessica
Broach, James R
Bolt, Michael
Moran, Jennifer
Fitzgerald, Dominic
Dileep, Vishnu
Liu, Tingting
Mei, Shenglin
Sasaki, Takayo
Trevilla-Garcia, Claudia
Wang, Su
Wang, Yanli
Zang, Chongzhi
Wang, Daifeng
Klein, Robert J.
Snyder, Michael
Gilbert, David M.
Yip, Kevin
Cheng, Chao
Yue, Feng
Liu, X. Shirley
White, Kevin P.
Gerstein, Mark
An integrative ENCODE resource for cancer genomics
title An integrative ENCODE resource for cancer genomics
title_full An integrative ENCODE resource for cancer genomics
title_fullStr An integrative ENCODE resource for cancer genomics
title_full_unstemmed An integrative ENCODE resource for cancer genomics
title_short An integrative ENCODE resource for cancer genomics
title_sort integrative encode resource for cancer genomics
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7391744/
https://www.ncbi.nlm.nih.gov/pubmed/32728046
http://dx.doi.org/10.1038/s41467-020-14743-w
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