Litcius/Paper detail

RNA Polymerase I Is Uniquely Vulnerable to the Small-Molecule Inhibitor BMH-21

Ruth Q. Jacobs, Kaila B. Fuller, Stephanie Cooper, Zachariah I. Carter, Marikki Laiho, Aaron L. Lucius, David A. Schneider

2022Cancers25 citationsDOIOpen Access PDF

Abstract

Cancer cells require robust ribosome biogenesis to maintain rapid cell growth during tumorigenesis. Because RNA polymerase I (Pol I) transcription of the ribosomal DNA (rDNA) is the first and rate-limiting step of ribosome biogenesis, it has emerged as a promising anti-cancer target. Over the last decade, novel cancer therapeutics targeting Pol I have progressed to clinical trials. BMH-21 is a first-in-class small molecule that inhibits Pol I transcription and represses cancer cell growth. Several recent studies have uncovered key mechanisms by which BMH-21 inhibits ribosome biosynthesis but the selectivity of BMH-21 for Pol I has not been directly measured. Here, we quantify the effects of BMH-21 on Pol I, RNA polymerase II (Pol II), and RNA polymerase III (Pol III) in vitro using purified components. We found that BMH-21 directly impairs nucleotide addition by Pol I, with no or modest effect on Pols II and III, respectively. Additionally, we found that BMH-21 does not affect the stability of any of the Pols' elongation complexes. These data demonstrate that BMH-21 directly exploits unique vulnerabilities of Pol I.

Topics & Concepts

ProcessivityRNA polymerase IRNA polymerase IIRNA polymerase IIIRibosome biogenesisDNA polymeraseTranscription (linguistics)Molecular biologyPolymeraseBiologyRNAChemistryRibosomeDNAGeneticsGene expressionRNA-dependent RNA polymeraseGenePromoterLinguisticsPhilosophyRNA modifications and cancerRNA and protein synthesis mechanismsGenomics and Chromatin Dynamics