Displacement of WDR5 from Chromatin by a WIN Site Inhibitor with Picomolar Affinity

Aho, Erin R.; Wang, J.; Gogliotti, Rocco D.; Howard, Gregory C.; Phan, Jason; Acharya, Pankaj; Macdonald, Jonathan D.; Cheng, Ken Chih-Chien; Lorey, Shelly L.; Lu, Binfeng; Wenzel, Sabine; Foshage, Audra M.; Alvarado, Joseph; Wang, Feng; Shaw, J. Grace; Zhao, Bin; Weissmiller, April M.; Thomas, Lance R.; Vakoc, Christopher R.; Hall, '; Hiebert, Scott W.; Liu, Q.; Stauffer, Shaun R.; Fesik, Stephen W.; Tansey, William P.

doi:10.1016/j.celrep.2019.02.047

Cited by 79 publications

(184 citation statements)

References 62 publications

(89 reference statements)

Supporting

Mentioning

173

Contrasting

Order By: Relevance

“…Gene ontology analyses revealed that most APC/C WDR5 target genes encode proteins involved in ribosome function (GO:0003735, p=1.2×10 −56 ) and mRNA translation (GO:0006413, p=2.2×10 −59 ). These genes are among the very first to be expressed upon mitotic exit 4 , dependent upon WDR5 and MYC 6 , 28 . Accordingly, APC/C WDR5 -target genes were strongly bound by the stem cell transcription factors MYC, OCT4, and NANOG ( Fig.…”

Section: Apc/c Acts At Transcription Start Sitesmentioning

confidence: 99%

Gene expression and cell identity controlled by anaphase-promoting complex

Mark

Mocciaro

et al. 2020

Nature

View full text Add to dashboard Cite

Metazoan development requires robust proliferation of progenitor cells, whose identities are established by tightly controlled transcriptional networks 1 . As gene expression is globally inhibited during mitosis, the transcriptional programs defining cell identity must be restarted in each cell cycle 2 - 5 , yet how this is accomplished is poorly understood. Here, we identified a ubiquitin-dependent mechanism that integrates gene expression with cell division to preserve cell identity. We found that WDR5 and TBP, which bind active interphase promoters 6 , 7 , recruit the anaphase-promoting complex (APC/C) to specific transcription start sites (TSS) during mitosis. This allows APC/C to decorate histones with K11/K48-branched ubiquitin chains that recruit p97/VCP and the proteasome and ensure rapid expression of pluripotency genes in the next cell cycle. Mitotic exit and transcription re-initiation are thus controlled by the same regulator, APC/C, which provides a robust mechanism to maintain cell identity through cell division.

show abstract

Section: Apc/c Acts At Transcription Start Sitesmentioning

confidence: 99%

Gene expression and cell identity controlled by anaphase-promoting complex

Mark

Mocciaro

et al. 2020

Nature

View full text Add to dashboard Cite

show abstract

“…WDR5 has a very discrete pattern of localization on chromatin, with narrow ChIP-Seq peaks that suggest focal recruitment to specific locations at target loci. 3,13 Within PSGs, the majority of these peaks occur just downstream of the transcription start site, and they are highly conserved in disparate cell types, 3 suggesting that both the binding of WDR5 to these genes, and its specific placement within them, is a precise and stably-determined event. Given the pattern of binding, it is entirely possible that placement of WDR5 on chromatin is driven by a sequence-specific DNA binding protein.…”

Section: The Insight: What Win Site Inhibitors Tell Us About Wdr5mentioning

confidence: 99%

“…A strong empirical case can be made that MLL-rearranged leukemia cells are sensitive to WIN site blockade, 3,9 and every indication is that WIN site inhibitors could be developed into effective treatments for MLL cancers. But the precise molecular underpinnings of this sensitivity remain unknown.…”

Section: The Promise: Clinical Utility Of Win Site Inhibitorsmentioning

confidence: 99%

Targeting WDR5: A WINning Anti-Cancer Strategy?

et al. 2019

View full text Add to dashboard Cite

WDR5 is a component of multiple epigenetic regulatory complexes, including the mixed lineage leukemia (MLL)/SET complexes that deposit histone H3 lysine 4 methylation. Inhibitors of an arginine-binding cavity in WDR5, known as the WDR5-interaction (WIN) site, have been proposed to selectively kill MLL-rearranged malignancies via an epigenetic mechanism. We discovered potent WIN site inhibitors and found that they kill MLL cancer cells not through changes in histone methylation, but by displacing WDR5 from chromatin at protein synthesis genes, choking the translational capacity of these cells, and inducing death via a nucleolar stress response. The mechanism of action of WIN site inhibitors reveals new aspects of WDR5 function and forecasts broad therapeutic utility as anti-cancer agents.

show abstract

“…Our recent studies have begun to overcome these obstacles. 8,9,10 In our most recent paper, 10 we studied the MYC-WDR5 connection in the context of Burkitt lymphoma, which is driven by a chromosomal translocation that places MYC expression under control of a potent immunoglobulin heavy chain enhancer. We learned that MYC and WDR5 co-bind to a fairly small group of genes that are manifestly connected to protein synthesis, including those encoding more than half of the proteins in the ribosome.…”

mentioning

confidence: 99%

“…In separate studies, 8 we discovered potent small molecule inhibitors against a second site on WDR5 known as the "WIN (WDR5-interaction) site" 6 ( Figure 1). WIN site inhibitors were originally discovered with the intention of treating leukemias bearing MLL1 gene rearrangements, and every indication is that they will have utility in that context.…”

mentioning

confidence: 99%

Targeting MYC through WDR5

Thomas

Adams

Fesik

et al. 2020

Molecular & Cellular Oncology

Self Cite

View full text Add to dashboard Cite

The oncoprotein transcription factor MYC is overexpressed in most cancers and is responsible for hundreds of thousands of cancer deaths worldwide every year. MYC is also a highly validatedbut currently undruggableanti-cancer target. We recently showed that breaking the interaction of MYC with its chromatin co-factor WD repeat-containing protein 5 (WDR5) promotes tumor regression in mouse xenografts, laying the foundation for a new strategy to inhibit MYC in the clinic.

show abstract

Displacement of WDR5 from Chromatin by a WIN Site Inhibitor with Picomolar Affinity

Cited by 79 publications

References 62 publications

Gene expression and cell identity controlled by anaphase-promoting complex

Gene expression and cell identity controlled by anaphase-promoting complex

Targeting WDR5: A WINning Anti-Cancer Strategy?

Targeting MYC through WDR5

Contact Info

Product

Resources

About