A DHODH inhibitor increases p53 synthesis and enhances tumor cell killing by p53 degradation blockage

DHODH抑制剂通过阻断p53降解,增加p53的合成并增强对肿瘤细胞的杀伤作用。

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作者:Marcus J G W Ladds ,Ingeborg M M van Leeuwen ,Catherine J Drummond ,Su Chu ,Alan R Healy ,Gergana Popova ,Andrés Pastor Fernández ,Tanzina Mollick ,Suhas Darekar ,Saikiran K Sedimbi ,Marta Nekulova ,Marijke C C Sachweh ,Johanna Campbell ,Maureen Higgins ,Chloe Tuck ,Mihaela Popa ,Mireia Mayoral Safont ,Pascal Gelebart ,Zinayida Fandalyuk ,Alastair M Thompson ,Richard Svensson ,Anna-Lena Gustavsson ,Lars Johansson ,Katarina Färnegårdh ,Ulrika Yngve ,Aljona Saleh ,Martin Haraldsson ,Agathe C A D'Hollander ,Marcela Franco ,Yan Zhao ,Maria Håkansson ,Björn Walse ,Karin Larsson ,Emma M Peat ,Vicent Pelechano ,John Lunec ,Borivoj Vojtesek ,Mar Carmena ,William C Earnshaw ,Anna R McCarthy ,Nicholas J Westwood ,Marie Arsenian-Henriksson ,David P Lane ,Ravi Bhatia ,Emmet McCormack ,Sonia Laín

Abstract

The development of non-genotoxic therapies that activate wild-type p53 in tumors is of great interest since the discovery of p53 as a tumor suppressor. Here we report the identification of over 100 small-molecules activating p53 in cells. We elucidate the mechanism of action of a chiral tetrahydroindazole (HZ00), and through target deconvolution, we deduce that its active enantiomer (R)-HZ00, inhibits dihydroorotate dehydrogenase (DHODH). The chiral specificity of HZ05, a more potent analog, is revealed by the crystal structure of the (R)-HZ05/DHODH complex. Twelve other DHODH inhibitor chemotypes are detailed among the p53 activators, which identifies DHODH as a frequent target for structurally diverse compounds. We observe that HZ compounds accumulate cancer cells in S-phase, increase p53 synthesis, and synergize with an inhibitor of p53 degradation to reduce tumor growth in vivo. We, therefore, propose a strategy to promote cancer cell killing by p53 instead of its reversible cell cycle arresting effect.

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