BRCA1 targets G2/M cell cycle proteins for ubiquitination and proteasomal degradation

S. Shabbeer; D. Omer; D. Berneman; O. Weitzman; A. Alpaugh; A. Pietraszkiewicz; S. Metsuyanim; A. Shainskaya; M. Z. Papa; R. I. Yarden

doi:10.1038/onc.2012.522

BRCA1 targets G2/M cell cycle proteins for ubiquitination and proteasomal degradation

S. Shabbeer, D. Omer, D. Berneman, O. Weitzman, A. Alpaugh, A. Pietraszkiewicz, S. Metsuyanim, A. Shainskaya, M. Z. Papa, R. I. Yarden

Weizmann Institute of Science

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

Abstract

The BRCA1 tumor suppressor protein heterodimerizes with its partner protein, BARD1, via the RING domain present in both proteins. The heterodimer contains an E3 ubiquitin ligase activity and participates in multiple cellular functions such as cell cycle control, DNA repair and regulation of gene transcription, collectively aimed at maintaining genomic stability and tumor suppression. Yet, the precise role of BRCA1 E3 ligase in these cellular functions is poorly understood. We present data showing that BRCA1 ubiquitinates G2/M cell cycle proteins, cyclin B and Cdc25C, leading to their accelerated degradation via a mechanism that is independent of APC/C. BRCA1-dependent degradation of cyclin B and Cdc25C is reversed by proteasome inhibitors and is enhanced following DNA damage, which may represent a possible mechanism to prevent cyclin B and Cdc25C accumulation, a requirement for mitotic entry. Our data provide mechanistic insight into how BRCA1 E3 ligase activity regulates the G2/M cell cycle checkpoint and, thus, contributes to maintenance of genomic stability.

Original language	English
Pages (from-to)	5005-5016
Number of pages	12
Journal	Oncogene
Volume	32
Issue number	42
DOIs	https://doi.org/10.1038/onc.2012.522
State	Published - Oct 2013

Keywords

BRCA1
Cdc25
Cyclin B
G2/M cell cycle checkpoint
Proteasome
Ubiquitination

All Science Journal Classification (ASJC) codes

Molecular Biology
Genetics
Cancer Research

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10.1038/onc.2012.522

Cite this

@article{d27225d8751a4d289a36aa2cb4baf0ab,

title = "BRCA1 targets G2/M cell cycle proteins for ubiquitination and proteasomal degradation",

abstract = "The BRCA1 tumor suppressor protein heterodimerizes with its partner protein, BARD1, via the RING domain present in both proteins. The heterodimer contains an E3 ubiquitin ligase activity and participates in multiple cellular functions such as cell cycle control, DNA repair and regulation of gene transcription, collectively aimed at maintaining genomic stability and tumor suppression. Yet, the precise role of BRCA1 E3 ligase in these cellular functions is poorly understood. We present data showing that BRCA1 ubiquitinates G2/M cell cycle proteins, cyclin B and Cdc25C, leading to their accelerated degradation via a mechanism that is independent of APC/C. BRCA1-dependent degradation of cyclin B and Cdc25C is reversed by proteasome inhibitors and is enhanced following DNA damage, which may represent a possible mechanism to prevent cyclin B and Cdc25C accumulation, a requirement for mitotic entry. Our data provide mechanistic insight into how BRCA1 E3 ligase activity regulates the G2/M cell cycle checkpoint and, thus, contributes to maintenance of genomic stability.",

keywords = "BRCA1, Cdc25, Cyclin B, G2/M cell cycle checkpoint, Proteasome, Ubiquitination",

author = "S. Shabbeer and D. Omer and D. Berneman and O. Weitzman and A. Alpaugh and A. Pietraszkiewicz and S. Metsuyanim and A. Shainskaya and Papa, \{M. Z.\} and Yarden, \{R. I.\}",

note = "Funding Information: We thank Drs B Henderson, J Pines, R Agami, E Rosen and M Brandeis for providing plasmids and Dr L Brody for reagents. We thank the microscopy unit in Bar-Ilan University for assistance with immunofluorescence studies and Dr I Goldstein and the flow cytometry unit at the Sheba medical center for assistance with fluorescence-activated cell sorting analysis. We thank Allison Hall for technical assistance. We thank Drs Eliot Rosen, Claire Pollack, Michael Brandeis and Gad Lavie for stimulating discussions and critical reading of the manuscript. This study was supported by a Research Career Development Award from the Israel Cancer Research Fund (to RIY) and by the funding from the Health Ministry (to RIY and MZP), the Israeli Cancer Association (RIY) and funds from Georgetown University, SNHS to RIY.",

year = "2013",

month = oct,

doi = "10.1038/onc.2012.522",

language = "الإنجليزيّة",

volume = "32",

pages = "5005--5016",

journal = "Oncogene",

issn = "0950-9232",

publisher = "Springer Nature",

number = "42",

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TY - JOUR

T1 - BRCA1 targets G2/M cell cycle proteins for ubiquitination and proteasomal degradation

AU - Shabbeer, S.

AU - Omer, D.

AU - Berneman, D.

AU - Weitzman, O.

AU - Alpaugh, A.

AU - Pietraszkiewicz, A.

AU - Metsuyanim, S.

AU - Shainskaya, A.

AU - Papa, M. Z.

AU - Yarden, R. I.

N1 - Funding Information: We thank Drs B Henderson, J Pines, R Agami, E Rosen and M Brandeis for providing plasmids and Dr L Brody for reagents. We thank the microscopy unit in Bar-Ilan University for assistance with immunofluorescence studies and Dr I Goldstein and the flow cytometry unit at the Sheba medical center for assistance with fluorescence-activated cell sorting analysis. We thank Allison Hall for technical assistance. We thank Drs Eliot Rosen, Claire Pollack, Michael Brandeis and Gad Lavie for stimulating discussions and critical reading of the manuscript. This study was supported by a Research Career Development Award from the Israel Cancer Research Fund (to RIY) and by the funding from the Health Ministry (to RIY and MZP), the Israeli Cancer Association (RIY) and funds from Georgetown University, SNHS to RIY.

PY - 2013/10

Y1 - 2013/10

N2 - The BRCA1 tumor suppressor protein heterodimerizes with its partner protein, BARD1, via the RING domain present in both proteins. The heterodimer contains an E3 ubiquitin ligase activity and participates in multiple cellular functions such as cell cycle control, DNA repair and regulation of gene transcription, collectively aimed at maintaining genomic stability and tumor suppression. Yet, the precise role of BRCA1 E3 ligase in these cellular functions is poorly understood. We present data showing that BRCA1 ubiquitinates G2/M cell cycle proteins, cyclin B and Cdc25C, leading to their accelerated degradation via a mechanism that is independent of APC/C. BRCA1-dependent degradation of cyclin B and Cdc25C is reversed by proteasome inhibitors and is enhanced following DNA damage, which may represent a possible mechanism to prevent cyclin B and Cdc25C accumulation, a requirement for mitotic entry. Our data provide mechanistic insight into how BRCA1 E3 ligase activity regulates the G2/M cell cycle checkpoint and, thus, contributes to maintenance of genomic stability.

AB - The BRCA1 tumor suppressor protein heterodimerizes with its partner protein, BARD1, via the RING domain present in both proteins. The heterodimer contains an E3 ubiquitin ligase activity and participates in multiple cellular functions such as cell cycle control, DNA repair and regulation of gene transcription, collectively aimed at maintaining genomic stability and tumor suppression. Yet, the precise role of BRCA1 E3 ligase in these cellular functions is poorly understood. We present data showing that BRCA1 ubiquitinates G2/M cell cycle proteins, cyclin B and Cdc25C, leading to their accelerated degradation via a mechanism that is independent of APC/C. BRCA1-dependent degradation of cyclin B and Cdc25C is reversed by proteasome inhibitors and is enhanced following DNA damage, which may represent a possible mechanism to prevent cyclin B and Cdc25C accumulation, a requirement for mitotic entry. Our data provide mechanistic insight into how BRCA1 E3 ligase activity regulates the G2/M cell cycle checkpoint and, thus, contributes to maintenance of genomic stability.

KW - BRCA1

KW - Cdc25

KW - Cyclin B

KW - G2/M cell cycle checkpoint

KW - Proteasome

KW - Ubiquitination

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U2 - 10.1038/onc.2012.522

DO - 10.1038/onc.2012.522

M3 - مقالة

SN - 0950-9232

VL - 32

SP - 5005

EP - 5016

JO - Oncogene

JF - Oncogene

IS - 42

ER -

BRCA1 targets G2/M cell cycle proteins for ubiquitination and proteasomal degradation

Abstract

Keywords

All Science Journal Classification (ASJC) codes

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