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2 research outputs found

Pharmacological inhibition of PRMT7 links arginine monomethylation to the cellular stress response

Author: Ackloo Suzanne
Al-Awar Rima
Aman Ahmed
Arrowsmith Cheryl H.
Baršytė-Lovejoy Dalia
Bonneil Eric
Brown Peter J.
Couzens Amber L.
dela Seña Carlo C.
Dilworth David
Eram Mohammad
Fukushi Hideto
Gingras Anne-Claude
Halabelian Levon
Harding Rachel
Hayashi Kozo
Ishikawa Yoshinori
Li Fengling
McLeod David
Nara Hiroshi
Organ Shawna
Richard Stephane
Sakai Nozomu
Sugo Tsukasa
Szewczyk Magdalena M.
Sánchez-Osuna Maria
Takagi Shinji
Takizawa Masayuki
Tyers Mike
Vedadi Masoud
Zepeda Carlos
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2020
Field of study

Protein arginine methyltransferases (PRMTs) regulate diverse biological processes and are increasingly being recognized for their potential as drug targets. Here we report the discovery of a potent, selective, and cell-active chemical probe for PRMT7. SGC3027 is a cell permeable prodrug, which in cells is converted to SGC8158, a potent, SAM-competitive PRMT7 inhibitor. Inhibition or knockout of cellular PRMT7 results in drastically reduced levels of arginine monomethylated HSP70 family stress-associated proteins. Structural and biochemical analyses reveal that PRMT7-driven in vitro methylation of HSP70 at R469 requires an ATP-bound, open conformation of HSP70. In cells, SGC3027 inhibits methylation of both constitutive and inducible forms of HSP70, and leads to decreased tolerance for perturbations of proteostasis including heat shock and proteasome inhibitors. These results demonstrate a role for PRMT7 and arginine methylation in stress response

Institutional Repository of Nature Research Centre

Discovery of a chemical probe for PRDM9

Author: Allali-Hassani Abdellah
Arrowsmith Cheryl H.
Baršytė-Lovejoy Dalia
Bennett D. Jonathan
Blazer Levi
Bok Jabez
Brown Peter J.
Dilworth David
Eram Mohammad S.
Gay Florence P. H.
Guccione Ernesto
Halabelian Levon
Ho Jessica Sook Yuin
Ivanochko Danton
Kaldis Philipp
Kattar Solomon D.
Li Fengling
Lima-Fernandes Evelyne
Loppnau Peter
Luciani Genna M.
Nicholson Benjamin
Organ Shawna L.
O’Hagan Ronan C.
Palmer Nathan
Sanders John M.
Schapira Matthieu
Szewczyk Magdalena M.
Talib S. Zakiah A.
Vedadi Masoud
Wu Qin
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2019
Field of study

PRDM9 is a PR domain containing protein which trimethylates histone 3 on lysine 4 and 36. Its normal expression is restricted to germ cells and attenuation of its activity results in altered meiotic gene transcription, impairment of double-stranded breaks and pairing between homologous chromosomes. There is growing evidence for a role of aberrant expression of PRDM9 in oncogenesis and genome instability. Here we report the discovery of MRK-740, a potent (IC50: 80 ± 16 nM), selective and cell-active PRDM9 inhibitor (Chemical Probe). MRK-740 binds in the substrate-binding pocket, with unusually extensive interactions with the cofactor S-adenosylmethionine (SAM), conferring SAM-dependent substrate-competitive inhibition. In cells, MRK-740 specifically and directly inhibits H3K4 methylation at endogenous PRDM9 target loci, whereas the closely related inactive control compound, MRK-740-NC, does not. The discovery of MRK-740 as a chemical probe for the PRDM subfamily of methyltransferases highlights the potential for exploiting SAM in targeting SAM-dependent methyltransferases

Lund University Publications

Institutional Repository of Nature Research Centre

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