Identification of a CARM1 Inhibitor with Potent In Vitro and In Vivo Activity in Preclinical Models of Multiple Myeloma

Drew, Allison E.; Moradei, Oscar; Jacques, Suzanne L.; Rioux, Nathalie; Boriack-Sjodin, Ann; Allain, Christina J.; Scott, Margaret Porter; Jin, Lei; Raimondi, Alejandra; Handler, Jessica L.; Ott, Heidi M.; Kruger, Ryan G.; McCabe, Michael T.; Sneeringer, Christopher J.; Riera, Thomas V.; Shapiro, Gideon; Waters, Nigel J.; Mitchell, Lorna H.; Duncan, Kenneth W.; Moyer, Mikel P.; Copeland, Robert A.; Smith, J. Joshua; Chesworth, Richard; Ribich, Scott

doi:10.1038/s41598-017-18446-z

Cited by 106 publications

(122 citation statements)

References 45 publications

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“…Competitive assays with SAM cofactor and peptide substrate showed that 2a and 5a act To the best of our knowledge, EZM2302, TP-064, SKI-73 (www.thesgc.org/chemicalprobes/SKI-73) and their derivatives are the only selective and cell-active CARM1 inhibitors. (Drew et al, 2017;Nakayama et al, 2018) While the potency, selectivity, on-target engagement and potential off-target effects associated with these compounds have been examined in vitro and in cellular contexts as chemical probes, EZM2302, TP-064, SKI-73 are distinct by their molecular scaffolds and modes of interaction with CARM1 (www.thesgc.org/chemical-probes/SKI-73). (Drew et al, 2017;Nakayama et al, 2018) SKI-73 is a cofactor analog inhibitor embedding a N6'homosinefungin moiety to engage the SAM binding site of CARM1 in a cofactor-competitive, substrate-noncompetitive manner; EZM2302 and TP-064 occupy the substrate-binding pocket of CARM1 in a SAH-uncompetitive or SAM-noncompetitive manner.…”

Section: Discussionmentioning

confidence: 99%

“…(Drew et al, 2017;Nakayama et al, 2018) While the potency, selectivity, on-target engagement and potential off-target effects associated with these compounds have been examined in vitro and in cellular contexts as chemical probes, EZM2302, TP-064, SKI-73 are distinct by their molecular scaffolds and modes of interaction with CARM1 (www.thesgc.org/chemical-probes/SKI-73). (Drew et al, 2017;Nakayama et al, 2018) SKI-73 is a cofactor analog inhibitor embedding a N6'homosinefungin moiety to engage the SAM binding site of CARM1 in a cofactor-competitive, substrate-noncompetitive manner; EZM2302 and TP-064 occupy the substrate-binding pocket of CARM1 in a SAH-uncompetitive or SAM-noncompetitive manner. (Drew et al, 2017;Nakayama et al, 2018) In particular, the prodrug property of SKI-73 allows its ready cellular uptake, followed by rapid conversion into its active forms inside cells.…”

Section: Discussionmentioning

confidence: 99%

“…(Blanc and Richard, 2017;Yang and Bedford, 2013) The requirement of CARM1 is implicated in multiple cancers with its methyltransferase activity particularly addicted by hematopoietic malignancies and metastatic breast cancer. (Drew et al, 2017;Greenblatt et al, 2018;Nakayama et al, 2018;Wang et al, 2014) Our prior efforts using in vivo mouse and in vitro cell models uncovered the role of CARM1 in promoting breast cancer metastasis. (Wang et al, 2014) Mechanistically, CARM1 methylates Arg1064 of BAF155 and thus facilitates the recruitment of the BAF155-containing SWI/SNF complex to a specific subset of gene loci essential for breast cancer metastasis.…”

Section: Introductionmentioning

confidence: 99%

“…(Wang et al, 2014) While this cancer relevance inspired the development of CARM1 inhibitors, (Kaniskan et al, 2018;Scheer et al, 2019) many small-molecule CARM1 inhibitors lack target selectivity or cellular activity (Kaniskan et al, 2018)---two essential criteria of chemical probes. (Frye, 2010) To the best of our knowledge, EZM2302, (Drew et al, 2017;Greenblatt et al, 2018) TP-064 (Nakayama et al, 2018) and SKI-73 (www.thesgc.org/chemical-probes/SKI-73) are the only selective and cell-active CARM1 chemical probes, which were developed by Epizyme, Takeda/SGC(Structural Genomic Consortium), and our team, respectively. EZM2302 and TP-064 were developed through conventional small-molecule scaffolds occupying the substrate-binding pocket of CARM1.…”

Section: Introductionmentioning

confidence: 99%

“…(Drew et al, 2017;Greenblatt et al, 2018;Nakayama et al, 2018) The potential utility of EZM2302 and TP-064 is implicated by their selective anti-proliferative effects on hematopoietic cancer cells, in particular multiple myeloma cells. (Drew et al, 2017;Greenblatt et al, 2018;Nakayama et al, 2018) However, definitive molecular mechanisms of the CARM1 addiction in these contexts remain elusive. (Greenblatt et al, 2018) Here we report the characterization and novel utility of SKI-73---a chemical probe of CARM1 with pro-drug properties.…”

Section: Introductionmentioning

confidence: 99%

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A Chemical Probe of CARM1 Alters Epigenetic Plasticity against Breast Cancer Cell Invasion

Cai

Zhang

Kim

et al. 2019

Preprint

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CARM1 is a cancer-relevant protein arginine methyltransferase that regulates many aspects of transcription. Its pharmacological inhibition is a promising anti-cancer strategy. Here SKI-73 is presented as a CARM1 chemical probe with pro-drug properties. SKI-73 can rapidly penetrate cell membranes and then be processed into active inhibitors, which are retained intracellularly with 10fold enrichment for days. These compounds were characterized for their potency, selectivity, modes of action, and on-target engagement. SKI-73 recapitulates the effect of CARM1 knockout against breast cancer cell invasion. Single-cell RNA-seq analysis revealed that the SKI-73-associated reduction of invasiveness act via altering epigenetic plasticity and suppressing the invasion-prone subpopulation. Interestingly, SKI-73 and CARM1 knockout alter the epigenetic plasticity with remarkable difference, arguing distinct modes of action between the small-molecule and genetic perturbation. We therefore discovered a CARM1-addiction mechanism of cancer metastasis and developed a chemical probe to target this process.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A Chemical Probe of CARM1 Alters Epigenetic Plasticity against Breast Cancer Cell Invasion

Cai

Zhang

Kim

et al. 2019

Preprint

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Looping forward: exploring R‐loop processing and therapeutic potential

Stratigi,

Siametis,

Garinis

2024

FEBS Letters

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Recently, there has been increasing interest in the complex relationship between transcription and genome stability, with specific attention directed toward the physiological significance of molecular structures known as R‐loops. These structures arise when an RNA strand invades into the DNA duplex, and their formation is involved in a wide range of regulatory functions affecting gene expression, DNA repair processes or cell homeostasis. The persistent presence of R‐loops, if not effectively removed, contributes to genome instability, underscoring the significance of the factors responsible for their resolution and modification. In this review, we provide a comprehensive overview of how R‐loop processing can drive either a beneficial or a harmful outcome. Additionally, we explore the potential for manipulating such structures to devise rationalized therapeutic strategies targeting the aberrant accumulation of R‐loops.

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Epigenetic Proteins as Emerging Drug Targets

Boriack-Sjodin

2020

Structural Biology in Drug Discovery

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Identification of a CARM1 Inhibitor with Potent In Vitro and In Vivo Activity in Preclinical Models of Multiple Myeloma

Cited by 106 publications

References 45 publications

A Chemical Probe of CARM1 Alters Epigenetic Plasticity against Breast Cancer Cell Invasion

A Chemical Probe of CARM1 Alters Epigenetic Plasticity against Breast Cancer Cell Invasion

Looping forward: exploring R‐loop processing and therapeutic potential

Epigenetic Proteins as Emerging Drug Targets

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