Ubiquitin ligation to F-box protein targets by SCF–RBR E3–E3 super-assembly

Horn‐Ghetko, Daniel; Krist, David T.; Prabu, J.R.; Baek, Kheewoong; Mulder, Monique P. C.; Klügel, Maren; Scott, Daniel C.; Ovaa, Huib; Kleiger, Gary; Schulman, Brenda A.

doi:10.1038/s41586-021-03197-9

Cited by 124 publications

(180 citation statements)

References 70 publications

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“…Most subunits of the APC/C, for example, are present throughout the cell cycle, but a combination of inhibitors and posttranslational modifications ensures that this E3 ligase ubiquitylates its targets during mitosis and in the subsequent G1 phase (Watson et al, 2019). The same applies to RBR family E3 ligases that often exist in autoinhibited conformations that are overcome by specific partners, including other E3 ligases or phosphorylated ubiquitin (Duda et al, 2013;Horn-Ghetko et al, 2021;Lechtenberg et al, 2016;Wauer et al, 2015). In addition, as shown for Cullin RING ligases, even expressed substrate adaptors do not form an active E3 ligase unless they have recognized their target and are allowed to engage the cullin scaffold in a process promoted by the exchange factor CAND1 (Liu et al, 2018;Pierce et al, 2013;Reichermeier et al, 2020).…”

Section: E3 Ligases At the Right Time And Placementioning

confidence: 99%

An E3 ligase guide to the galaxy of small-molecule-induced protein degradation

Jevtić

Haakonsen

Rapé

2021

Cell Chemical Biology

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Section: E3 Ligases At the Right Time And Placementioning

confidence: 99%

An E3 ligase guide to the galaxy of small-molecule-induced protein degradation

Jevtić

Haakonsen

Rapé

2021

Cell Chemical Biology

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“…Cyclin F was combined with neddylated Cul1, Skp1, substrate, and ubiquitin. The human homologue of ariadne ( ARIH1) is a RING-Between-RING (RBR) E3 ligase that has been shown to work with the E2 UBCH7 and other cullin ring E3 ligases, including the SCF, to ubiquitinate substrates (Horn-Ghetko et al, 2021;Scott et al, 2016). Therefore, ARIH1/UBCH7 and the chainelongating E2 CDC34b were used as the ubiquitin transfer module.…”

Section: P130 Is a Cyclin F Substratementioning

confidence: 99%

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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“…As last speaker of this session, Klaus Rumpel from Boehringer Ingelheim (BI) presented findings from BIs BCL6 inhibitor program, where he and his colleagues surprisingly identified BCL6‐degrading compounds [5] . These compounds have been very influential in the field and most recently where shown to induce BCL6 polymerization ultimately leading to degradation [6] . Taken together, contributions by Thomä, Schulman and Rumpel were highly stimulating for the audience and their findings will be important to the vibrant field of targeted protein degradation.…”

Section: Opening Lecturementioning

confidence: 99%

Med Chem Remote: The Frontiers in Medicinal Chemistry 2021

et al. 2021

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Digital, but delicious! The Frontiers in Medicinal Chemistry 2021 meeting, originally intended to take place in Darmstadt, carried on as an online event from March 8–10 this year. Even with pandemic restrictions, the event co‐presented by the Medicinal Chemistry Division of the German Chemical Society (GDCh), the German Pharmaceutical Society (DPhG), and the Swiss Chemical Society (SCS) proved to be a success, showcasing excellent speakers and facilitating participant interaction in an ingenious virtual setting. Over 350 participants from more than 10 countries gathered to discuss the latest trends and directions in medicinal chemistry, with sessions on molecular glues, covalent fragments, transient binding pockets and more. This report presents a summary of the key lectures and activities at the event.

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Ubiquitin ligation to F-box protein targets by SCF–RBR E3–E3 super-assembly

Cited by 124 publications

References 70 publications

An E3 ligase guide to the galaxy of small-molecule-induced protein degradation

An E3 ligase guide to the galaxy of small-molecule-induced protein degradation

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

Med Chem Remote: The Frontiers in Medicinal Chemistry 2021

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