Transcriptional Heterogeneity Overcomes Super-Enhancer Disrupting Drug Combinations in Multiple Myeloma.

Seth J Welsh ,Victoria M Garbitt ,Sochilt Brown ,Sagar Lonial ,Kennedi Todd ,Nicklus H Cuc ,Benjamin G Barwick ,Lawrence H Boise ,Nathalie Meurice ,Paola Neri ,Leslie D Abrego Rocha ,Yuliza Tafoya Alvarado ,Camille Herzog ,Chang-Xin Shi ,Zachary J Hammond ,Wei Liao ,Caleb K Stein ,Erin W Meermeier ,Courtney Wittenberg ,Meaghen E Sharik ,Yuan Xiao Zhu ,Joachim Petit ,Daniel L Riggs ,Peng Li ,Warren J Leonard ,Wei-Dong D Chen ,Nizar J Bahlis ,Anna V Roschke ,Rodrigo Fonseca-Portilla ,Yulia N Demchenko ,Megan T Du ,Marta Chesi ,P Leif Bergsagel

doi:10.1158/2643-3230.bcd-23-0062

Transcriptional Heterogeneity Overcomes Super-Enhancer Disrupting Drug Combinations in Multiple Myeloma.

Seth J Welsh , Victoria M Garbitt + Show 31 more

Open Access

https://doi.org/10.1158/2643-3230.bcd-23-0062

Copy DOI

Journal: Blood Cancer Discovery	Publication Date: Sep 27, 2023
Citations: 4	License type: CC BY-NC-ND 4.0

Affiliation: Mayo Clinic, Emory University, University of Calgary, Tulane University, National Heart Lung and Blood Institute, Center for Cancer Research

#Multiple Myeloma #Related Article + Show 8 more

Abstract
Full-Text PDF
Similar Papers

Abstract

These results highlight the dependence of MM on IKZF1-bound super-enhancers, which can be effectively targeted by a potent therapeutic combination pairing IMiD-mediated degradation of IKZF1 and IKZF3 with EP300 inhibition. They also identify AP-1 factors as an unrecognized mechanism of IMiD resistance in MM. See related article by Neri, Barwick, et al., p. 56. See related commentary by Yun and Cleveland, p. 5. This article is featured in Selected Articles from This Issue, p. 4.

Full Text