RNF20 Inhibits TFIIS-Facilitated Transcriptional Elongation to Suppress Pro-oncogenic Gene Expression

Efrat Shema; Jaehoon Kim; Robert G. Roeder; Moshe Oren

doi:10.1016/j.molcel.2011.03.011

RNF20 Inhibits TFIIS-Facilitated Transcriptional Elongation to Suppress Pro-oncogenic Gene Expression

Efrat Shema, Jaehoon Kim, Robert G. Roeder, Moshe Oren

Department of Molecular Cell Biology

Weizmann Institute of Science

Research output: Contribution to journal › Article › peer-review

Abstract

hBRE1/RNF20 is the major E3 ubiquitin ligase for histone H2B. RNF20 depletion causes a global reduction of monoubiquitylated H2B (H2Bub) levels and augments the expression of growth-promoting, pro-oncogenic genes. Those genes reside preferentially in compact chromatin and are inefficiently transcribed under basal conditions. We now report that RNF20, presumably via H2Bub, selectively represses those genes by interfering with chromatin recruitment of TFIIS, a factor capable of relieving stalled RNA polymerase II. RNF20 inhibits the interaction between TFIIS and the PAF1 complex and hinders transcriptional elongation. TFIIS ablation selectively abolishes the upregulation of those genes upon RNF20 depletion and attenuates the cellular response to EGF. Consistent with its positive role in transcription of pro-oncogenic genes, TFIIS expression is elevated in various human tumors. Our findings provide a molecular mechanism for selective gene repression by RNF20 and position TFIIS as a key target of RNF20's tumor suppressor activity.

Original language	English
Pages (from-to)	477-488
Number of pages	12
Journal	Molecular Cell
Volume	42
Issue number	4
DOIs	https://doi.org/10.1016/j.molcel.2011.03.011
State	Published - 20 May 2011

All Science Journal Classification (ASJC) codes

Molecular Biology
Cell Biology

Access to Document

10.1016/j.molcel.2011.03.011

Cite this

@article{2a08c847953245c4afcb4ba674b1e9f2,

title = "RNF20 Inhibits TFIIS-Facilitated Transcriptional Elongation to Suppress Pro-oncogenic Gene Expression",

abstract = "hBRE1/RNF20 is the major E3 ubiquitin ligase for histone H2B. RNF20 depletion causes a global reduction of monoubiquitylated H2B (H2Bub) levels and augments the expression of growth-promoting, pro-oncogenic genes. Those genes reside preferentially in compact chromatin and are inefficiently transcribed under basal conditions. We now report that RNF20, presumably via H2Bub, selectively represses those genes by interfering with chromatin recruitment of TFIIS, a factor capable of relieving stalled RNA polymerase II. RNF20 inhibits the interaction between TFIIS and the PAF1 complex and hinders transcriptional elongation. TFIIS ablation selectively abolishes the upregulation of those genes upon RNF20 depletion and attenuates the cellular response to EGF. Consistent with its positive role in transcription of pro-oncogenic genes, TFIIS expression is elevated in various human tumors. Our findings provide a molecular mechanism for selective gene repression by RNF20 and position TFIIS as a key target of RNF20's tumor suppressor activity.",

author = "Efrat Shema and Jaehoon Kim and Roeder, \{Robert G.\} and Moshe Oren",

note = "National Cancer Institute [R37 CA40099, CA129325, DK071900]; Dr. Miriam and Sheldon Adelson Medical Research Foundation; Lower Saxony-Israeli Association; Yad Abraham Center for Cancer Diagnosis and Therapy; Israel Academy of Sciences and HumanitiesWe thank Gilad Fuchs, Itay Tirosh, Yael Aylon, Lior Golomb, and Efrat Lidor-Nili for great help and stimulating discussions. This work was supported in part by grant R37 CA40099 (to M.O.) and grants CA129325 and DK071900 (to R.G.R.) from the National Cancer Institute, the Dr. Miriam and Sheldon Adelson Medical Research Foundation, The Lower Saxony-Israeli Association, and the Yad Abraham Center for Cancer Diagnosis and Therapy. M.O. is incumbent of the Andre Lwoff chair in Molecular Biology. E.S. is supported by the Adams Fellowship Program of the Israel Academy of Sciences and Humanities. J.K. is a senior fellow of the Charles H. Revson Foundation.",

year = "2011",

month = may,

day = "20",

doi = "10.1016/j.molcel.2011.03.011",

language = "الإنجليزيّة",

volume = "42",

pages = "477--488",

journal = "Molecular Cell",

issn = "1097-2765",

publisher = "Cell Press",

number = "4",

}

TY - JOUR

T1 - RNF20 Inhibits TFIIS-Facilitated Transcriptional Elongation to Suppress Pro-oncogenic Gene Expression

AU - Shema, Efrat

AU - Kim, Jaehoon

AU - Roeder, Robert G.

AU - Oren, Moshe

N1 - National Cancer Institute [R37 CA40099, CA129325, DK071900]; Dr. Miriam and Sheldon Adelson Medical Research Foundation; Lower Saxony-Israeli Association; Yad Abraham Center for Cancer Diagnosis and Therapy; Israel Academy of Sciences and HumanitiesWe thank Gilad Fuchs, Itay Tirosh, Yael Aylon, Lior Golomb, and Efrat Lidor-Nili for great help and stimulating discussions. This work was supported in part by grant R37 CA40099 (to M.O.) and grants CA129325 and DK071900 (to R.G.R.) from the National Cancer Institute, the Dr. Miriam and Sheldon Adelson Medical Research Foundation, The Lower Saxony-Israeli Association, and the Yad Abraham Center for Cancer Diagnosis and Therapy. M.O. is incumbent of the Andre Lwoff chair in Molecular Biology. E.S. is supported by the Adams Fellowship Program of the Israel Academy of Sciences and Humanities. J.K. is a senior fellow of the Charles H. Revson Foundation.

PY - 2011/5/20

Y1 - 2011/5/20

N2 - hBRE1/RNF20 is the major E3 ubiquitin ligase for histone H2B. RNF20 depletion causes a global reduction of monoubiquitylated H2B (H2Bub) levels and augments the expression of growth-promoting, pro-oncogenic genes. Those genes reside preferentially in compact chromatin and are inefficiently transcribed under basal conditions. We now report that RNF20, presumably via H2Bub, selectively represses those genes by interfering with chromatin recruitment of TFIIS, a factor capable of relieving stalled RNA polymerase II. RNF20 inhibits the interaction between TFIIS and the PAF1 complex and hinders transcriptional elongation. TFIIS ablation selectively abolishes the upregulation of those genes upon RNF20 depletion and attenuates the cellular response to EGF. Consistent with its positive role in transcription of pro-oncogenic genes, TFIIS expression is elevated in various human tumors. Our findings provide a molecular mechanism for selective gene repression by RNF20 and position TFIIS as a key target of RNF20's tumor suppressor activity.

AB - hBRE1/RNF20 is the major E3 ubiquitin ligase for histone H2B. RNF20 depletion causes a global reduction of monoubiquitylated H2B (H2Bub) levels and augments the expression of growth-promoting, pro-oncogenic genes. Those genes reside preferentially in compact chromatin and are inefficiently transcribed under basal conditions. We now report that RNF20, presumably via H2Bub, selectively represses those genes by interfering with chromatin recruitment of TFIIS, a factor capable of relieving stalled RNA polymerase II. RNF20 inhibits the interaction between TFIIS and the PAF1 complex and hinders transcriptional elongation. TFIIS ablation selectively abolishes the upregulation of those genes upon RNF20 depletion and attenuates the cellular response to EGF. Consistent with its positive role in transcription of pro-oncogenic genes, TFIIS expression is elevated in various human tumors. Our findings provide a molecular mechanism for selective gene repression by RNF20 and position TFIIS as a key target of RNF20's tumor suppressor activity.

UR - http://www.scopus.com/inward/record.url?scp=79955946995&partnerID=8YFLogxK

U2 - 10.1016/j.molcel.2011.03.011

DO - 10.1016/j.molcel.2011.03.011

M3 - مقالة

SN - 1097-2765

VL - 42

SP - 477

EP - 488

JO - Molecular Cell

JF - Molecular Cell

IS - 4

ER -

RNF20 Inhibits TFIIS-Facilitated Transcriptional Elongation to Suppress Pro-oncogenic Gene Expression

Abstract

All Science Journal Classification (ASJC) codes

Access to Document

Other files and links

Fingerprint

Cite this