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Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome

Organization of the genome into euchromatin and heterochromatin appears to be evolutionarily conserved and relatively stable during lineage differentiation. In an effort to unravel the basic principle underlying genome folding, here we focus on the genome itself and report a fundamental role for L1...

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Autores principales: Lu, J. Yuyang, Chang, Lei, Li, Tong, Wang, Ting, Yin, Yafei, Zhan, Ge, Han, Xue, Zhang, Ke, Tao, Yibing, Percharde, Michelle, Wang, Liang, Peng, Qi, Yan, Pixi, Zhang, Hui, Bi, Xianju, Shao, Wen, Hong, Yantao, Wu, Zhongyang, Ma, Runze, Wang, Peizhe, Li, Wenzhi, Zhang, Jing, Chang, Zai, Hou, Yingping, Zhu, Bing, Ramalho-Santos, Miguel, Li, Pilong, Xie, Wei, Na, Jie, Sun, Yujie, Shen, Xiaohua
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Singapore 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8169921/
https://www.ncbi.nlm.nih.gov/pubmed/33514913
http://dx.doi.org/10.1038/s41422-020-00466-6
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author Lu, J. Yuyang
Chang, Lei
Li, Tong
Wang, Ting
Yin, Yafei
Zhan, Ge
Han, Xue
Zhang, Ke
Tao, Yibing
Percharde, Michelle
Wang, Liang
Peng, Qi
Yan, Pixi
Zhang, Hui
Bi, Xianju
Shao, Wen
Hong, Yantao
Wu, Zhongyang
Ma, Runze
Wang, Peizhe
Li, Wenzhi
Zhang, Jing
Chang, Zai
Hou, Yingping
Zhu, Bing
Ramalho-Santos, Miguel
Li, Pilong
Xie, Wei
Na, Jie
Sun, Yujie
Shen, Xiaohua
author_facet Lu, J. Yuyang
Chang, Lei
Li, Tong
Wang, Ting
Yin, Yafei
Zhan, Ge
Han, Xue
Zhang, Ke
Tao, Yibing
Percharde, Michelle
Wang, Liang
Peng, Qi
Yan, Pixi
Zhang, Hui
Bi, Xianju
Shao, Wen
Hong, Yantao
Wu, Zhongyang
Ma, Runze
Wang, Peizhe
Li, Wenzhi
Zhang, Jing
Chang, Zai
Hou, Yingping
Zhu, Bing
Ramalho-Santos, Miguel
Li, Pilong
Xie, Wei
Na, Jie
Sun, Yujie
Shen, Xiaohua
author_sort Lu, J. Yuyang
collection PubMed
description Organization of the genome into euchromatin and heterochromatin appears to be evolutionarily conserved and relatively stable during lineage differentiation. In an effort to unravel the basic principle underlying genome folding, here we focus on the genome itself and report a fundamental role for L1 (LINE1 or LINE-1) and B1/Alu retrotransposons, the most abundant subclasses of repetitive sequences, in chromatin compartmentalization. We find that homotypic clustering of L1 and B1/Alu demarcates the genome into grossly exclusive domains, and characterizes and predicts Hi-C compartments. Spatial segregation of L1-rich sequences in the nuclear and nucleolar peripheries and B1/Alu-rich sequences in the nuclear interior is conserved in mouse and human cells and occurs dynamically during the cell cycle. In addition, de novo establishment of L1 and B1 nuclear segregation is coincident with the formation of higher-order chromatin structures during early embryogenesis and appears to be critically regulated by L1 and B1 transcripts. Importantly, depletion of L1 transcripts in embryonic stem cells drastically weakens homotypic repeat contacts and compartmental strength, and disrupts the nuclear segregation of L1- or B1-rich chromosomal sequences at genome-wide and individual sites. Mechanistically, nuclear co-localization and liquid droplet formation of L1 repeat DNA and RNA with heterochromatin protein HP1α suggest a phase-separation mechanism by which L1 promotes heterochromatin compartmentalization. Taken together, we propose a genetically encoded model in which L1 and B1/Alu repeats blueprint chromatin macrostructure. Our model explains the robustness of genome folding into a common conserved core, on which dynamic gene regulation is overlaid across cells.
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spelling pubmed-81699212021-06-07 Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome Lu, J. Yuyang Chang, Lei Li, Tong Wang, Ting Yin, Yafei Zhan, Ge Han, Xue Zhang, Ke Tao, Yibing Percharde, Michelle Wang, Liang Peng, Qi Yan, Pixi Zhang, Hui Bi, Xianju Shao, Wen Hong, Yantao Wu, Zhongyang Ma, Runze Wang, Peizhe Li, Wenzhi Zhang, Jing Chang, Zai Hou, Yingping Zhu, Bing Ramalho-Santos, Miguel Li, Pilong Xie, Wei Na, Jie Sun, Yujie Shen, Xiaohua Cell Res Article Organization of the genome into euchromatin and heterochromatin appears to be evolutionarily conserved and relatively stable during lineage differentiation. In an effort to unravel the basic principle underlying genome folding, here we focus on the genome itself and report a fundamental role for L1 (LINE1 or LINE-1) and B1/Alu retrotransposons, the most abundant subclasses of repetitive sequences, in chromatin compartmentalization. We find that homotypic clustering of L1 and B1/Alu demarcates the genome into grossly exclusive domains, and characterizes and predicts Hi-C compartments. Spatial segregation of L1-rich sequences in the nuclear and nucleolar peripheries and B1/Alu-rich sequences in the nuclear interior is conserved in mouse and human cells and occurs dynamically during the cell cycle. In addition, de novo establishment of L1 and B1 nuclear segregation is coincident with the formation of higher-order chromatin structures during early embryogenesis and appears to be critically regulated by L1 and B1 transcripts. Importantly, depletion of L1 transcripts in embryonic stem cells drastically weakens homotypic repeat contacts and compartmental strength, and disrupts the nuclear segregation of L1- or B1-rich chromosomal sequences at genome-wide and individual sites. Mechanistically, nuclear co-localization and liquid droplet formation of L1 repeat DNA and RNA with heterochromatin protein HP1α suggest a phase-separation mechanism by which L1 promotes heterochromatin compartmentalization. Taken together, we propose a genetically encoded model in which L1 and B1/Alu repeats blueprint chromatin macrostructure. Our model explains the robustness of genome folding into a common conserved core, on which dynamic gene regulation is overlaid across cells. Springer Singapore 2021-01-29 2021-06 /pmc/articles/PMC8169921/ /pubmed/33514913 http://dx.doi.org/10.1038/s41422-020-00466-6 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/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/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Article
Lu, J. Yuyang
Chang, Lei
Li, Tong
Wang, Ting
Yin, Yafei
Zhan, Ge
Han, Xue
Zhang, Ke
Tao, Yibing
Percharde, Michelle
Wang, Liang
Peng, Qi
Yan, Pixi
Zhang, Hui
Bi, Xianju
Shao, Wen
Hong, Yantao
Wu, Zhongyang
Ma, Runze
Wang, Peizhe
Li, Wenzhi
Zhang, Jing
Chang, Zai
Hou, Yingping
Zhu, Bing
Ramalho-Santos, Miguel
Li, Pilong
Xie, Wei
Na, Jie
Sun, Yujie
Shen, Xiaohua
Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title_full Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title_fullStr Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title_full_unstemmed Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title_short Homotypic clustering of L1 and B1/Alu repeats compartmentalizes the 3D genome
title_sort homotypic clustering of l1 and b1/alu repeats compartmentalizes the 3d genome
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8169921/
https://www.ncbi.nlm.nih.gov/pubmed/33514913
http://dx.doi.org/10.1038/s41422-020-00466-6
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