Unbiased transcriptome signature of in vivo cell proliferation reveals pro- and antiproliferative gene networks

Meital Cohen; Manuela Vecsler; Arthur Liberzon; Meirav Noach; Eitan Zlotorynski; Amit Tzur

doi:10.4161/cc.26030

Unbiased transcriptome signature of in vivo cell proliferation reveals pro- and antiproliferative gene networks

Meital Cohen, Manuela Vecsler, Arthur Liberzon, Meirav Noach, Eitan Zlotorynski, Amit Tzur

The Mina and Everard Goodman Faculty of Life Sciences

Bar-Ilan University

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

Abstract

Different types of mature B-cell lymphocytes are overall highly similar. Nevertheless, some B cells proliferate intensively, while others rarely do. Here, we demonstrate that a simple binary classification of gene expression in proliferating vs. resting B cells can identify, with remarkable selectivity, global in vivo regulators of the mammalian cell cycle, many of which are also post-translationally regulated by the APC/C E3 ligase. Consequently, we discover a novel regulatory network between the APC/C and the E2F transcription factors and discuss its potential impact on the G₁-S transition of the cell cycle. In addition, by focusing on genes whose expression inversely correlates with proliferation, we demonstrate the inherent ability of our approach to also identify in vivo regulators of cell differentiation, cell survival, and other antiproliferative processes. Relying on data sets of wt, non-transgenic animals, our approach can be applied to other cell lineages and human data sets.

Original language	English
Pages (from-to)	2992-3000
Number of pages	9
Journal	Cell Cycle
Volume	12
Issue number	18
DOIs	https://doi.org/10.4161/cc.26030
State	Published - 15 Sep 2013

Keywords

APC
APC/C
Atypical E2Fs
Cdh1
Cell cycle
Differentiation
E2F1
E2F7
E2F8
Proliferation
Sur vival
Transcriptome
Ubiquitin

All Science Journal Classification (ASJC) codes

Molecular Biology
Developmental Biology
Cell Biology

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title = "Unbiased transcriptome signature of in vivo cell proliferation reveals pro- and antiproliferative gene networks",

abstract = "Different types of mature B-cell lymphocytes are overall highly similar. Nevertheless, some B cells proliferate intensively, while others rarely do. Here, we demonstrate that a simple binary classification of gene expression in proliferating vs. resting B cells can identify, with remarkable selectivity, global in vivo regulators of the mammalian cell cycle, many of which are also post-translationally regulated by the APC/C E3 ligase. Consequently, we discover a novel regulatory network between the APC/C and the E2F transcription factors and discuss its potential impact on the G1-S transition of the cell cycle. In addition, by focusing on genes whose expression inversely correlates with proliferation, we demonstrate the inherent ability of our approach to also identify in vivo regulators of cell differentiation, cell survival, and other antiproliferative processes. Relying on data sets of wt, non-transgenic animals, our approach can be applied to other cell lineages and human data sets.",

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author = "Meital Cohen and Manuela Vecsler and Arthur Liberzon and Meirav Noach and Eitan Zlotorynski and Amit Tzur",

note = "Funding Information: We are deeply indebted to Dr Jane Seagal for introducing us to the wonders of immunology, and to Prof Doron Ginsberg for reagents. Funding by the Israeli Centers of Research Excellence (I-CORE), Gene Regulation in Complex Human Disease, Center No. 41/11 (AT); the Israel Cancer Association Grant 20120067 (AT); the German–Israeli Foundation (GIF), No. 2294-2269.2/2011 (AT); and the Israel Cancer Research Fund (ICRF) postdoctoral fellowship (MV) is gratefully acknowledged.",

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doi = "10.4161/cc.26030",

language = "الإنجليزيّة",

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AU - Zlotorynski, Eitan

AU - Tzur, Amit

N1 - Funding Information: We are deeply indebted to Dr Jane Seagal for introducing us to the wonders of immunology, and to Prof Doron Ginsberg for reagents. Funding by the Israeli Centers of Research Excellence (I-CORE), Gene Regulation in Complex Human Disease, Center No. 41/11 (AT); the Israel Cancer Association Grant 20120067 (AT); the German–Israeli Foundation (GIF), No. 2294-2269.2/2011 (AT); and the Israel Cancer Research Fund (ICRF) postdoctoral fellowship (MV) is gratefully acknowledged.

PY - 2013/9/15

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N2 - Different types of mature B-cell lymphocytes are overall highly similar. Nevertheless, some B cells proliferate intensively, while others rarely do. Here, we demonstrate that a simple binary classification of gene expression in proliferating vs. resting B cells can identify, with remarkable selectivity, global in vivo regulators of the mammalian cell cycle, many of which are also post-translationally regulated by the APC/C E3 ligase. Consequently, we discover a novel regulatory network between the APC/C and the E2F transcription factors and discuss its potential impact on the G1-S transition of the cell cycle. In addition, by focusing on genes whose expression inversely correlates with proliferation, we demonstrate the inherent ability of our approach to also identify in vivo regulators of cell differentiation, cell survival, and other antiproliferative processes. Relying on data sets of wt, non-transgenic animals, our approach can be applied to other cell lineages and human data sets.

AB - Different types of mature B-cell lymphocytes are overall highly similar. Nevertheless, some B cells proliferate intensively, while others rarely do. Here, we demonstrate that a simple binary classification of gene expression in proliferating vs. resting B cells can identify, with remarkable selectivity, global in vivo regulators of the mammalian cell cycle, many of which are also post-translationally regulated by the APC/C E3 ligase. Consequently, we discover a novel regulatory network between the APC/C and the E2F transcription factors and discuss its potential impact on the G1-S transition of the cell cycle. In addition, by focusing on genes whose expression inversely correlates with proliferation, we demonstrate the inherent ability of our approach to also identify in vivo regulators of cell differentiation, cell survival, and other antiproliferative processes. Relying on data sets of wt, non-transgenic animals, our approach can be applied to other cell lineages and human data sets.

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Unbiased transcriptome signature of in vivo cell proliferation reveals pro- and antiproliferative gene networks

Abstract

Keywords

All Science Journal Classification (ASJC) codes

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