Cell cycle oscillators underlying orderly proteolysis of E2F8

Wasserman, Danit; Nachum, Sapir; Cohen, Meital; Enrico, Taylor P; Noach-Hirsh, Meirav; Parasol, Jasmin; Zomer-Polak, Sarit; Auerbach, Naomi; Sheinberger-Chorni, Evelin; Nevenzal, Hadas; Levi-Dadon, Nofar; Wang, Xianxi; Lahmi, Roxane; Michaely, Efrat; Gerber, Doron; Emanuele, Michael J.; Tzur, Amit

doi:10.1101/672964

Cited by 4 publications

(4 citation statements)

References 67 publications

(18 reference statements)

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“…We detected an interaction between the two proteins, irrespective of which protein was precipitated (Figure 8, I and J), suggesting that E2F8 binds Cyclin F. Taken together, these data suggest that E2F8 regulation by Cyclin F is direct and that SCF Cyclin F activity downregulates E2F8 prior to M-phase entry. These data (see also Wasserman et al, 2019) complement three parallel studies connecting SCF Cyclin F -mediated proteolysis to temporal dynamics of E2F members (Burdova et al, 2019;Clijsters et al, 2019;Yuan et al, 2019).…”

Section: E2f8 Is Regulated By the F-box Protein Cyclin Fsupporting

confidence: 76%

Cell cycle oscillators underlying orderly proteolysis of E2F8

Wasserman

Nachum

Cohen

et al. 2020

MBoC

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Section: E2f8 Is Regulated By the F-box Protein Cyclin Fsupporting

confidence: 76%

Cell cycle oscillators underlying orderly proteolysis of E2F8

Wasserman

Nachum

Cohen

et al. 2020

MBoC

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“…We next examined endogenous proteins corresponding to the CDK-RB network genes that correlate most strongly with CCNF . We used two breast cancer cell lines, MCF-7 and T47D, engineered for doxycycline-inducible expression of cyclin F (Wasserman et al, 2020). Cells were treated with increasing amounts of doxycycline for 24 hours, then harvested for immunoblot to determine levels of CDK4, CDK6, cyclin D1, p107, and p130.…”

Section: Resultsmentioning

confidence: 99%

“…The ubiquitination of activator E2Fs allows for their degradation, and expression of mutant E2Fs that can no longer bind to cyclin F results in increased expression of E2F target genes. Further, during G2 phase, cyclin F was shown to regulate the atypical repressor E2Fs, E2F7 and E2F8, promoting their degradation(Wasserman et al, 2020; Yuan et al, 2019). Each of these substrates implicate cyclin F in indirectly controlling cell cycle gene expression, and our study uncovers a new mechanism by which cyclin F regulates transcriptional control at the start of the cell cycle, by ubiquitinating p130.…”

Section: Discussionmentioning

confidence: 99%

“…Further, cyclin F is involved in cell cycle gene transcription both through its non-catalytic inhibition of B-MYB after DNA damage (Klein et al, 2015), and its ubiquitination of activator and repressor E2Fs (Burdova et al, 2019; Clijsters et al, 2019; Wasserman et al, 2020; Yuan et al, 2019) and the stem-loop binding protein (SLBP) in G2-phase (Dankert et al, 2016). Together, its dynamic cell cycle regulation and numerous cell cycle substrates highlight the importance of cyclin F in cell cycle control.…”

Section: Introductionmentioning

confidence: 99%

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Cyclin F drives proliferation through SCF-dependent degradation of the retinoblastoma-like tumor suppressor p130/RBL2

Enrico

Stallaert

Wick

et al. 2021

Preprint

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Cell cycle gene expression programs fuel proliferation and are dysregulated in many cancers. The retinoblastoma-family proteins, RB, p130/RBL2 and p107/RBL1, coordinately repress cell cycle gene expression, inhibiting proliferation and suppressing tumorigenesis. Ubiquitin-dependent protein degradation is essential to cell cycle control, and numerous proliferative regulators, tumor suppressors, and oncoproteins are ubiquitinated. However, little is known about the role of ubiquitin signaling in controlling RB-family proteins. A systems genetics analysis of several hundred CRISPR/Cas9 loss-of-function screens suggested the potential regulation of the RB-network by cyclin F, a substrate recognition receptor for the SCF family of E3 ligases. We demonstrate that RBL2/p130 is a direct substrate of SCFcyclin F. We map a cyclin F regulatory site to a flexible linker in the p130 pocket domain, and show that this site mediates binding, stability, and ubiquitination. Expression of a non-degradable p130 represses cell cycle gene expression and strongly reduces proliferation. These data suggest that SCFcyclin Fplays a key role in the CDK-RB network and raises the possibility that aberrant p130 degradation could dysregulate the cell cycle in human cancers.

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