The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22

Timothy J. Stanek; Victoria J. Gennaro; Mason A. Tracewell; Daniela Di Marcantonio; Kristen L. Pauley; Sabrina Butt; Christopher McNair; Feng Wang; Andrew V. Kossenkov; Karen E. Knudsen; Tauseef Butt; Stephen M. Sykes; Steven B. McMahon

doi:10.15252/embj.2019102509

The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22

Timothy J. Stanek, Victoria J. Gennaro, Mason A. Tracewell, Daniela Di Marcantonio, Kristen L. Pauley, Sabrina Butt, Christopher McNair, Feng Wang, Andrew V. Kossenkov, Karen E. Knudsen, Tauseef Butt, Stephen M. Sykes, Steven B. McMahon^*

^*此作品的通讯作者

科研成果: 期刊稿件 › 文章 › 同行评审

9 引用（Scopus）

摘要

The SAGA coactivator complex is essential for eukaryotic transcription and comprises four distinct modules, one of which contains the ubiquitin hydrolase USP22. In yeast, the USP22 ortholog deubiquitylates H2B, resulting in Pol II Ser2 phosphorylation and subsequent transcriptional elongation. In contrast to this H2B-associated role in transcription, we report here that human USP22 contributes to the early stages of stimulus-responsive transcription, where USP22 is required for pre-initiation complex (PIC) stability. Specifically, USP22 maintains long-range enhancer–promoter contacts and controls loading of Mediator tail and general transcription factors (GTFs) onto promoters, with Mediator core recruitment being USP22-independent. In addition, we identify Mediator tail subunits MED16 and MED24 and the Pol II subunit RBP1 as potential non-histone substrates of USP22. Overall, these findings define a role for human SAGA within the earliest steps of transcription.

源语言	英语
文章编号	e102509
期刊	EMBO Journal
卷	40
期	16
DOI	https://doi.org/10.15252/embj.2019102509
出版状态	已出版 - 16 8月 2021
已对外发布	是

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Stanek, T. J., Gennaro, V. J., Tracewell, M. A., Di Marcantonio, D., Pauley, K. L., Butt, S., McNair, C., Wang, F., Kossenkov, A. V., Knudsen, K. E., Butt, T., Sykes, S. M., & McMahon, S. B. (2021). The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22. EMBO Journal, 40(16), 文章 e102509. https://doi.org/10.15252/embj.2019102509

@article{e43d3723c41e49ba9abf9959d8954f4f,

title = "The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22",

abstract = "The SAGA coactivator complex is essential for eukaryotic transcription and comprises four distinct modules, one of which contains the ubiquitin hydrolase USP22. In yeast, the USP22 ortholog deubiquitylates H2B, resulting in Pol II Ser2 phosphorylation and subsequent transcriptional elongation. In contrast to this H2B-associated role in transcription, we report here that human USP22 contributes to the early stages of stimulus-responsive transcription, where USP22 is required for pre-initiation complex (PIC) stability. Specifically, USP22 maintains long-range enhancer–promoter contacts and controls loading of Mediator tail and general transcription factors (GTFs) onto promoters, with Mediator core recruitment being USP22-independent. In addition, we identify Mediator tail subunits MED16 and MED24 and the Pol II subunit RBP1 as potential non-histone substrates of USP22. Overall, these findings define a role for human SAGA within the earliest steps of transcription.",

keywords = "SAGA, USP22, epigenetic, pre-initiation complex, transcription",

author = "Stanek, {Timothy J.} and Gennaro, {Victoria J.} and Tracewell, {Mason A.} and {Di Marcantonio}, Daniela and Pauley, {Kristen L.} and Sabrina Butt and Christopher McNair and Feng Wang and Kossenkov, {Andrew V.} and Knudsen, {Karen E.} and Tauseef Butt and Sykes, {Stephen M.} and McMahon, {Steven B.}",

note = "Publisher Copyright: {\textcopyright} 2021 The Authors. Published under the terms of the CC BY NC ND 4.0 license",

year = "2021",

month = aug,

day = "16",

doi = "10.15252/embj.2019102509",

language = "English",

volume = "40",

journal = "EMBO Journal",

issn = "0261-4189",

publisher = "Springer Science and Business Media Deutschland GmbH",

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T1 - The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22

AU - Stanek, Timothy J.

AU - Gennaro, Victoria J.

AU - Tracewell, Mason A.

AU - Di Marcantonio, Daniela

AU - Pauley, Kristen L.

AU - Butt, Sabrina

AU - McNair, Christopher

AU - Wang, Feng

AU - Kossenkov, Andrew V.

AU - Knudsen, Karen E.

AU - Butt, Tauseef

AU - Sykes, Stephen M.

AU - McMahon, Steven B.

PY - 2021/8/16

Y1 - 2021/8/16

N2 - The SAGA coactivator complex is essential for eukaryotic transcription and comprises four distinct modules, one of which contains the ubiquitin hydrolase USP22. In yeast, the USP22 ortholog deubiquitylates H2B, resulting in Pol II Ser2 phosphorylation and subsequent transcriptional elongation. In contrast to this H2B-associated role in transcription, we report here that human USP22 contributes to the early stages of stimulus-responsive transcription, where USP22 is required for pre-initiation complex (PIC) stability. Specifically, USP22 maintains long-range enhancer–promoter contacts and controls loading of Mediator tail and general transcription factors (GTFs) onto promoters, with Mediator core recruitment being USP22-independent. In addition, we identify Mediator tail subunits MED16 and MED24 and the Pol II subunit RBP1 as potential non-histone substrates of USP22. Overall, these findings define a role for human SAGA within the earliest steps of transcription.

AB - The SAGA coactivator complex is essential for eukaryotic transcription and comprises four distinct modules, one of which contains the ubiquitin hydrolase USP22. In yeast, the USP22 ortholog deubiquitylates H2B, resulting in Pol II Ser2 phosphorylation and subsequent transcriptional elongation. In contrast to this H2B-associated role in transcription, we report here that human USP22 contributes to the early stages of stimulus-responsive transcription, where USP22 is required for pre-initiation complex (PIC) stability. Specifically, USP22 maintains long-range enhancer–promoter contacts and controls loading of Mediator tail and general transcription factors (GTFs) onto promoters, with Mediator core recruitment being USP22-independent. In addition, we identify Mediator tail subunits MED16 and MED24 and the Pol II subunit RBP1 as potential non-histone substrates of USP22. Overall, these findings define a role for human SAGA within the earliest steps of transcription.

KW - SAGA

KW - USP22

KW - epigenetic

KW - pre-initiation complex

KW - transcription

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DO - 10.15252/embj.2019102509

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AN - SCOPUS:85108263090

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VL - 40

JO - EMBO Journal

JF - EMBO Journal

IS - 16

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ER -

The SAGA complex regulates early steps in transcription via its deubiquitylase module subunit USP22

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