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Polycomb Associates Genome-wide with a Specific RNA Polymerase II Variant, and Regulates Metabolic Genes in ESCs

Polycomb Associates Genome-wide with a Specific RNA Polymerase II Variant, and Regulates Metabolic Genes in ESCs
Polycomb Associates Genome-wide with a Specific RNA Polymerase II Variant, and Regulates Metabolic Genes in ESCs
Polycomb repressor complexes (PRCs) are important chromatin modifiers fundamentally implicated in pluripotency and cancer. Polycomb silencing in embryonic stem cells (ESCs) can be accompanied by active chromatin and primed RNA polymerase II (RNAPII), but the relationship between PRCs and RNAPII remains unclear genome-wide. We mapped PRC repression markers and four RNAPII states in ESCs using ChIP-seq, and found that PRC targets exhibit a range of RNAPII variants. First, developmental PRC targets are bound by unproductive RNAPII (S5p+S7p−S2p−) genome-wide. Sequential ChIP, Ring1B depletion, and genome-wide correlations show that PRCs and RNAPII-S5p physically bind to the same chromatin and functionally synergize. Second, we identify a cohort of genes marked by PRC and elongating RNAPII (S5p+S7p+S2p+); they produce mRNA and protein, and their expression increases upon PRC1 knockdown. We show that this group of PRC targets switches between active and PRC-repressed states within the ESC population, and that many have roles in metabolism.
1934-5909
157-170
Brookes, Emily
425dafc2-111b-4f6c-9336-f720c4ef8cac
de Santiago, Inês
0796d468-5e1a-452c-abc2-ecbd57456f56
Hebenstreit, Daniel
1bebcdf4-bf4d-4e5d-ba25-1b954cd60c3a
Morris, Kelly J.
e05ef5d6-4038-445e-9f42-5a66b723f842
Carroll, Tom
0f316034-8504-42db-bdac-d0fae840b997
Xie, Sheila Q.
166026b3-727f-41e8-aeec-309bf846737c
Stock, Julie K.
61eb7d6c-e011-4572-aff2-510bfc6a1231
Heidemann, Martin
0ee80f6a-faf0-4b24-8d32-599baaed61bd
Eick, Dirk
b120f206-7d81-4417-9610-823f57e1a677
Nozaki, Naohito
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Kimura, Hiroshi
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Ragoussis, Jiannis
ce3c01bb-38e4-47cb-b74c-d8ec92cc8da4
Teichmann, Sarah Amalia
09635869-f0d3-4ead-aa38-bf3975c4c977
Pombo, Ana
9ea8d0ea-3ec6-43d4-92d5-d1754994a366
Brookes, Emily
425dafc2-111b-4f6c-9336-f720c4ef8cac
de Santiago, Inês
0796d468-5e1a-452c-abc2-ecbd57456f56
Hebenstreit, Daniel
1bebcdf4-bf4d-4e5d-ba25-1b954cd60c3a
Morris, Kelly J.
e05ef5d6-4038-445e-9f42-5a66b723f842
Carroll, Tom
0f316034-8504-42db-bdac-d0fae840b997
Xie, Sheila Q.
166026b3-727f-41e8-aeec-309bf846737c
Stock, Julie K.
61eb7d6c-e011-4572-aff2-510bfc6a1231
Heidemann, Martin
0ee80f6a-faf0-4b24-8d32-599baaed61bd
Eick, Dirk
b120f206-7d81-4417-9610-823f57e1a677
Nozaki, Naohito
3e33e844-9a47-4805-8c3d-8b04279463d7
Kimura, Hiroshi
fd455010-0d1c-4e3e-b8ef-e311afc65c7b
Ragoussis, Jiannis
ce3c01bb-38e4-47cb-b74c-d8ec92cc8da4
Teichmann, Sarah Amalia
09635869-f0d3-4ead-aa38-bf3975c4c977
Pombo, Ana
9ea8d0ea-3ec6-43d4-92d5-d1754994a366

Brookes, Emily, de Santiago, Inês, Hebenstreit, Daniel, Morris, Kelly J., Carroll, Tom, Xie, Sheila Q., Stock, Julie K., Heidemann, Martin, Eick, Dirk, Nozaki, Naohito, Kimura, Hiroshi, Ragoussis, Jiannis, Teichmann, Sarah Amalia and Pombo, Ana (2012) Polycomb Associates Genome-wide with a Specific RNA Polymerase II Variant, and Regulates Metabolic Genes in ESCs. Cell Stem Cell, 10 (2), 157-170. (doi:10.1016/j.stem.2011.12.017).

Record type: Article

Abstract

Polycomb repressor complexes (PRCs) are important chromatin modifiers fundamentally implicated in pluripotency and cancer. Polycomb silencing in embryonic stem cells (ESCs) can be accompanied by active chromatin and primed RNA polymerase II (RNAPII), but the relationship between PRCs and RNAPII remains unclear genome-wide. We mapped PRC repression markers and four RNAPII states in ESCs using ChIP-seq, and found that PRC targets exhibit a range of RNAPII variants. First, developmental PRC targets are bound by unproductive RNAPII (S5p+S7p−S2p−) genome-wide. Sequential ChIP, Ring1B depletion, and genome-wide correlations show that PRCs and RNAPII-S5p physically bind to the same chromatin and functionally synergize. Second, we identify a cohort of genes marked by PRC and elongating RNAPII (S5p+S7p+S2p+); they produce mRNA and protein, and their expression increases upon PRC1 knockdown. We show that this group of PRC targets switches between active and PRC-repressed states within the ESC population, and that many have roles in metabolism.

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Published date: 1 February 2012

Identifiers

Local EPrints ID: 472121
URI: http://eprints.soton.ac.uk/id/eprint/472121
ISSN: 1934-5909
PURE UUID: 8eff9807-c43a-404e-9a19-2be65270d4e8
ORCID for Emily Brookes: ORCID iD orcid.org/0000-0003-2175-4349

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Date deposited: 28 Nov 2022 17:34
Last modified: 17 Mar 2024 04:14

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Contributors

Author: Emily Brookes ORCID iD
Author: Inês de Santiago
Author: Daniel Hebenstreit
Author: Kelly J. Morris
Author: Tom Carroll
Author: Sheila Q. Xie
Author: Julie K. Stock
Author: Martin Heidemann
Author: Dirk Eick
Author: Naohito Nozaki
Author: Hiroshi Kimura
Author: Jiannis Ragoussis
Author: Sarah Amalia Teichmann
Author: Ana Pombo

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