1. Academic Validation
  2. Design, synthesis and biological evaluation of matrine contains benzimidazole derivatives as dual TOPOI and PARP inhibitors for cancer therapy

Design, synthesis and biological evaluation of matrine contains benzimidazole derivatives as dual TOPOI and PARP inhibitors for cancer therapy

  • Eur J Med Chem. 2024 Mar 27:270:116348. doi: 10.1016/j.ejmech.2024.116348.
Gan Qiu 1 Junwei Xie 2 Fan Li 2 Keyan Han 1 Qingfeng Long 2 Jamal A H Kowah 1 Ruobing Gao 2 Lisheng Wang 3 Xu Liu 4
Affiliations

Affiliations

  • 1 School of Chemistry and Chemical Engineering, Guangxi University, Nanning, 530004, China.
  • 2 School of Medicine, Guangxi University, Nanning, 530004, China.
  • 3 School of Medicine, Guangxi University, Nanning, 530004, China. Electronic address: lswang@gxu.edu.cn.
  • 4 School of Medicine, Guangxi University, Nanning, 530004, China. Electronic address: wendaoliuxu@163.com.
Abstract

TOPOI inhibitors have long been a focal point in the research and development of antitumor drugs. PARP-1 plays a crucial role in repairing DNA damage induced by TOPOI inhibitors. Thus, concurrent inhibition of TOPOI and PARP-1 has the potential to augment drug activity. Matrine, characterized by low toxicity and good water solubility, offers advantageous properties. In this investigation, a series of benzimidazole matrine derivatives were designed and synthesized using matrine as the lead compound with the aim of developing dual inhibitors targeting both TOPOI and PARP-1. Among these derivatives, Compound B6 exhibited potent inhibitory effects on PARP-1 and TOPOI, effectively suppressing Cancer cell proliferation and migration. Mechanistic assessments revealed that B6 induced DNA damage in HGC-27 cells, leading to G0/G1 cell cycle arrest and significant Apoptosis. Molecular docking experiments demonstrated that B6 can effectively enter the active pocket of target proteins, where it forms stable hydrogen bonds with amino acid residues. In vivo, experiments demonstrated that B6 exhibited antitumor activity comparable to that of the positive control drug. The tumor growth inhibition rates (TGIs) for irinotecan, B6 and matrine were 87.0%, 75.4% and 9.7%, respectively. Importantly, B6 demonstrated lower toxicity than the positive control drug. Our findings suggest that TOPOI and PARP-1 may represent potential targets for matrine and B6 emerges as a promising candidate for Cancer therapy.

Keywords

Cancer; DNA damage; Matrine derivatives; PARP; TOPOI.

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