Marikki Laiho scite author profile

SUMMARY We define here the activity and mechanisms of action of a small molecule lead compound for cancer targeting. We show that the compound, BMH-21, has wide and potent antitumorigenic activity across NCI60 cancer cell lines and represses tumor growth in vivo. BMH-21 binds GC-rich sequences, which is present at high frequency in ribosomal DNA genes, and potently and rapidly represses RNA polymerase I (Pol I) transcription. Strikingly, we find that BMH-21 causes proteasome-dependent destruction of RPA194, the large catalytic subunit protein of Pol I holocomplex, and this correlates with cancer cell killing. Our results show that Pol I activity is under proteasome-mediated control, which reveals an unexpected therapeutic opportunity.

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Marikki Laiho

TGFβ signals through a heteromeric protein kinase receptor complex

Growth inhibition by TGF-β linked to suppression of retinoblastoma protein phosphorylation

A Targeting Modality for Destruction of RNA Polymerase I that Possesses Anticancer Activity

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