Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition

The chromatin-associated protein WDR5 is a promising target for cancer drug discovery, with most efforts blocking an arginine-binding cavity on the protein called the “WIN” site that tethers WDR5 to chromatin. WIN site inhibitors (WINi) are active against multiple cancer cell types in vitro, the mos...

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Autores principales: Howard, Gregory C., Wang, Jing, Rose, Kristie Lindsey, Patel, Purvi, Tsui, Tina, Florian, Andrea C., Lorey, Shelly L., Grieb, Brian C., Smith, Brianna N., Slota, Macey J., Reynolds, Elizabeth M., Goswami, Soumita, Savona, Michael R., Lee, Taekyu, Fesik, Stephen W., Liu, Qi, Tansey, William P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10402127/
https://www.ncbi.nlm.nih.gov/pubmed/37546802
http://dx.doi.org/10.1101/2023.07.26.550648
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author Howard, Gregory C.
Wang, Jing
Rose, Kristie Lindsey
Patel, Purvi
Tsui, Tina
Florian, Andrea C.
Lorey, Shelly L.
Grieb, Brian C.
Smith, Brianna N.
Slota, Macey J.
Reynolds, Elizabeth M.
Goswami, Soumita
Savona, Michael R.
Lee, Taekyu
Fesik, Stephen W.
Liu, Qi
Tansey, William P.
author_facet Howard, Gregory C.
Wang, Jing
Rose, Kristie Lindsey
Patel, Purvi
Tsui, Tina
Florian, Andrea C.
Lorey, Shelly L.
Grieb, Brian C.
Smith, Brianna N.
Slota, Macey J.
Reynolds, Elizabeth M.
Goswami, Soumita
Savona, Michael R.
Lee, Taekyu
Fesik, Stephen W.
Liu, Qi
Tansey, William P.
author_sort Howard, Gregory C.
collection PubMed
description The chromatin-associated protein WDR5 is a promising target for cancer drug discovery, with most efforts blocking an arginine-binding cavity on the protein called the “WIN” site that tethers WDR5 to chromatin. WIN site inhibitors (WINi) are active against multiple cancer cell types in vitro, the most notable of which are those derived from MLL-rearranged (MLLr) leukemias. Peptidomimetic WINi were originally proposed to inhibit MLLr cells via dysregulation of genes connected to hematopoetic stem cell expansion. Our discovery and interrogation of small molecule WIN site inhibitors, however, revealed that they act in MLLr cell lines to suppress ribosome protein gene (RPG) transcription, induce nucleolar stress, and activate p53. Because there is no precedent for an anti-cancer strategy that specifically targets RPG expression, we took an integrated multi-omics approach to further interrogate the mechanism of action of WINi in MLLr cancer cells. We show that WINi induce depletion of the stock of ribosomes, accompanied by a broad translational choke, induction of a DNA damage response, and changes in alternative mRNA splicing that inactivate the p53 antagonist MDM4. We also show that WINi are synergistic with agents including venetoclax and BET-bromodomain inhibitors. Together, these studies reinforce the concept that WINi are a novel type of ribosome-directed anti-cancer therapy and provide a resource to support their clinical implementation in MLLr leukemias and other malignancies.
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spelling pubmed-104021272023-08-05 Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition Howard, Gregory C. Wang, Jing Rose, Kristie Lindsey Patel, Purvi Tsui, Tina Florian, Andrea C. Lorey, Shelly L. Grieb, Brian C. Smith, Brianna N. Slota, Macey J. Reynolds, Elizabeth M. Goswami, Soumita Savona, Michael R. Lee, Taekyu Fesik, Stephen W. Liu, Qi Tansey, William P. bioRxiv Article The chromatin-associated protein WDR5 is a promising target for cancer drug discovery, with most efforts blocking an arginine-binding cavity on the protein called the “WIN” site that tethers WDR5 to chromatin. WIN site inhibitors (WINi) are active against multiple cancer cell types in vitro, the most notable of which are those derived from MLL-rearranged (MLLr) leukemias. Peptidomimetic WINi were originally proposed to inhibit MLLr cells via dysregulation of genes connected to hematopoetic stem cell expansion. Our discovery and interrogation of small molecule WIN site inhibitors, however, revealed that they act in MLLr cell lines to suppress ribosome protein gene (RPG) transcription, induce nucleolar stress, and activate p53. Because there is no precedent for an anti-cancer strategy that specifically targets RPG expression, we took an integrated multi-omics approach to further interrogate the mechanism of action of WINi in MLLr cancer cells. We show that WINi induce depletion of the stock of ribosomes, accompanied by a broad translational choke, induction of a DNA damage response, and changes in alternative mRNA splicing that inactivate the p53 antagonist MDM4. We also show that WINi are synergistic with agents including venetoclax and BET-bromodomain inhibitors. Together, these studies reinforce the concept that WINi are a novel type of ribosome-directed anti-cancer therapy and provide a resource to support their clinical implementation in MLLr leukemias and other malignancies. Cold Spring Harbor Laboratory 2023-07-29 /pmc/articles/PMC10402127/ /pubmed/37546802 http://dx.doi.org/10.1101/2023.07.26.550648 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Howard, Gregory C.
Wang, Jing
Rose, Kristie Lindsey
Patel, Purvi
Tsui, Tina
Florian, Andrea C.
Lorey, Shelly L.
Grieb, Brian C.
Smith, Brianna N.
Slota, Macey J.
Reynolds, Elizabeth M.
Goswami, Soumita
Savona, Michael R.
Lee, Taekyu
Fesik, Stephen W.
Liu, Qi
Tansey, William P.
Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title_full Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title_fullStr Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title_full_unstemmed Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title_short Ribosome subunit attrition and activation of the p53–MDM4 axis dominate the response of MLL-rearranged cancer cells to WDR5 WIN site inhibition
title_sort ribosome subunit attrition and activation of the p53–mdm4 axis dominate the response of mll-rearranged cancer cells to wdr5 win site inhibition
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10402127/
https://www.ncbi.nlm.nih.gov/pubmed/37546802
http://dx.doi.org/10.1101/2023.07.26.550648
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