Abstract
Ubiquitin-specific protease 11 (USP11) is a promising anticancer target, but selective inhibitor development has proved to be challenging. Here, we designed and synthesized selective USP11 inhibitors based on a previously reported covalent probe (N-benzyl-4-(2-chloroacetyl)-1-methyl-1H-pyrrole-2-carboxamide, compound 2) that is a more potent inhibitor of USP4 than USP11. Compound 7, derived from 2 by the introduction of a piperidine moiety, exhibited an IC(50) of 2.59 μM, while the replacement of chloroacetyl with a methyl sulfonylpiperazine moiety (compound 26) displayed equivalent potency. Sustained inhibition of USP11 consistent with covalent binding was observed in a jump dilution assay, and the compounds displayed significantly lower activity against the paralogues USP4 and USP15. Both compounds inhibited the proliferation of PEO4 ovarian and MDA-MB-231 breast cancer cells. Notably, compound 26 displayed cytostatic activity, and normal fibroblast MRC-5 cells were less affected. The findings highlight the potential of 7 and 26 as promising candidates for the development of selective tool compounds and therapeutic agents targeting USP11.