TAS4464, A Highly Potent and Selective Inhibitor of NEDD8-Activating Enzyme, Suppresses Neddylation and Shows Antitumor Activity in Diverse Cancer Models.

Chihoko Yoshimura,Shingo Tsuji,Yu Komiya,Toru Takenaka,Shuichi Ohkubo,Naoya Fujita,Hiroaki Ochiiwa,Hiromi Muraoka,Akihiro Hashimoto,Fumio Nakagawa,Hiromi Kazuno,Satoshi Suzuki,Takashi Mizutani,Masafumi Kumazaki

doi:10.1158/1535-7163.mct-18-0644

Chihoko Yoshimura, Shingo Tsuji + Show 12 more

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https://doi.org/10.1158/1535-7163.mct-18-0644

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Journal: Molecular cancer therapeutics	Publication Date: Jul 1, 2019
Citations: 46	License type: cc-by

Affiliation: Taiho Pharmaceutical (Japan)

Abstract

NEDD8-activating enzyme (NAE) is an essential E1 enzyme of the NEDD8 conjugation (neddylation) pathway, which controls cancer cell growth and survival through activation of cullin-RING ubiquitin ligase complexes (CRL). In this study, we describe the preclinical profile of a novel, highly potent, and selective NAE inhibitor, TAS4464. TAS4464 selectively inhibited NAE relative to the other E1s UAE and SAE. TAS4464 treatment inhibited cullin neddylation and subsequently induced the accumulation of CRL substrates such as CDT1, p27, and phosphorylated IκBα in human cancer cell lines. TAS4464 showed greater inhibitory effects than those of the known NAE inhibitor MLN4924 both in enzyme assay and in cells. Cytotoxicity profiling revealed that TAS4464 is highly potent with widespread antiproliferative activity not only for cancer cell lines, but also patient-derived tumor cells. TAS4464 showed prolonged target inhibition in human tumor xenograft mouse models; weekly or twice a week TAS4464 administration led to prominent antitumor activity in multiple human tumor xenograft mouse models including both hematologic and solid tumors without marked weight loss. As a conclusion, TAS4464 is the most potent and highly selective NAE inhibitor reported to date, showing superior antitumor activity with prolonged target inhibition. It is, therefore, a promising agent for the treatment of a variety of tumors including both hematologic and solid tumors. These results support the clinical evaluation of TAS4464 in hematologic and solid tumors.

Highlights

The ubiquitin-like modifier NEDD8 controls the stability and activity of its target proteins via a conjugation cascade
TAS4464 is a highly potent and selective inhibitor of NEDD8-activating enzyme (NAE) TAS4464 was discovered by means of library screening and structure-based design (Fig. 1A) and its synthetic procedure is described in Supplementary Fig. S1
We hypothesized that TAS4464 creates a covalent adduct with NEDD8 on NAE due to its sulfonamide structure, which is reported to be the key element to create the covalent bond between an inhibitor and Ubl on E1 enzymes in an ATP-dependent manner [35, 36]

Summary

Introduction

The ubiquitin-like modifier NEDD8 controls the stability and activity of its target proteins via a conjugation cascade (the neddylation pathway; ref. 1). The ubiquitin-like modifier NEDD8 controls the stability and activity of its target proteins via a conjugation cascade NEDD8-activating enzyme (NAE; a heterodimer of APP-BP1 and UBA3), an E1 enzyme, is a key regulator of the neddylation pathway. NAE starts the neddylation pathway by the transfer NEDD8 to its E2 enzyme UBE2M called as UBC12; UAE (an E1 enzyme) transfers Ub to UBE2C (an E2 enzyme) in the ubiquitination pathway and SAE (an E1 enzyme) transfers SUMO1 to UBE2I (an E2 enzyme) in the SUMOylation pathway [2, 3]. Overexpression of NEDD8 and NAE is reported in multiple types of cancer [4,5,6,7], and elevated levels of NEDD8 transcripts are reported to correlate with the poor prognosis of patients with bortezomib-treated multiple. Note: Supplementary data for this article are available at Molecular Cancer Therapeutics Online (http://mct.aacrjournals.org/)

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