AUTHOR=Zhang Xiaoyi , Jiang Lingna , Li Yixin , Feng Qiqi , Sun Xiulin , Wang Yaonan , Zhao Ming 

TITLE=Discovery of novel benzylquinazoline molecules as p97/VCP inhibitors

JOURNAL=Frontiers in Pharmacology

VOLUME=14

YEAR=2023

URL=https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2023.1209060

DOI=10.3389/fphar.2023.1209060

ISSN=1663-9812

ABSTRACT=<p><bold>Introduction:</bold> Protein p97 is an extensively investigated AAA ATPase with various cellular activities, including cell cycle control, ubiquitin–proteasome system, autophagy, and NF-κB activation.</p><p><bold>Method:</bold> In this study, we designed, synthesized and evaluated eight novel DBeQanalogs as potential p97 inhibitors <italic>in vivo</italic> and <italic>in vitro</italic>.</p><p><bold>Results:</bold> In the p97 ATPase inhibition assay, compounds <bold>6</bold> and <bold>7</bold> showed higher potency than the known p97 inhibitors, DBeQ and CB-5083. Compounds <bold>4-6</bold> dramatically induced G0/G1 phase arrest in the HCT116 cells, and compound <bold>7</bold> arrested the cells in both G0/G1 and S phases. Western blots showed elevated levels of SQSTM/p62, ATF-4, and NF-κB in HCT116 cells with the treatment of compounds <bold>4–7</bold>, confirming their role in inhibiting the p97 signaling pathway in cells. In addition, the IC<sub>50</sub> of compounds <bold>4–6</bold> against HCT116, RPMI-8226, and s180 proliferation were 0.24–6.9 µM with comparable potency as DBeQ. However, compounds <bold>4–6</bold> displayed low toxicity against the normal human colon cell line. Thus, compounds <bold>6</bold> and <bold>7</bold> were proved to be potential p97 inhibitors with less cytotoxicity. <italic>In vivo</italic> studies using the s180 xenograft model have demonstrated that compound <bold>6</bold> inhibited tumor growth, led to a significant reduction of p97 concentration in the serum and tumor, and indicated non-toxicity on the body weight and organ-to-brain weight ratios except for the spleen at the dose of 90 μmol/kg/day for 10 days. Furthermore, the present study indicated that compound <bold>6</bold> may not induce s180 mice myelosuppression often observed in the p97 inhibitors.</p><p><bold>Conclusion:</bold> Compound <bold>6</bold> displayed high binding affinity to p97, great p97 ATPase inhibition, selective cytotoxicity, remarkable anti-tumor effect, and upregulated safety, which improved the clinical potential of p97 inhibitors.</p>