New Natural Eugenol Derivatives as Antiproliferative Agents: Synthesis, Biological Evaluation, and Computational Studies

被引:22
|
作者
Nazreen, Syed [1 ]
Elbehairi, Serag Eldin I. [2 ,3 ]
Malebari, Azizah M. [4 ]
Alghamdi, Nuha [1 ]
Alshehri, Reem F. [5 ]
Shati, Ali A. [2 ]
Ali, Nada M. [1 ]
Alfaifi, Mohammad Y. [2 ]
Elhenawy, Ahmed A. [6 ]
Alam, Mohammad Mahboob [1 ]
机构
[1] Al Baha Univ, Fac Sci, Dept Chem, Al Baha 65799, Saudi Arabia
[2] King Khalid Univ, Fac Sci, Dept Biol, Abha 9004, Saudi Arabia
[3] VACSERA Holding Co, Egyptian Org Biol Prod & Vaccines, Cell Culture Lab, Giza 2311, Egypt
[4] King Abdulaziz Univ, Fac Pharm, Dept Pharmaceut Chem, Jeddah 21589, Saudi Arabia
[5] Taibah Univ, Fac Sci & Art, Chem Dept, Madinah 16857, Saudi Arabia
[6] Al Azhar Unuvers, Fac Sci, Chem Dept, Cairo 11751, Egypt
来源
ACS OMEGA | 2023年 / 8卷 / 21期
关键词
MOLECULAR DOCKING; MOIETY; INHIBITORS;
D O I
10.1021/acsomega.3c00933
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Semisynthetic modifications of natural products havebestowed uswith many anticancer drugs. In the present work, a natural product,eugenol, has been modified synthetically to generate new anticanceragents. The final compounds were structurally confirmed by NMR, IR,and mass techniques. From the cytotoxicity results, compound 17 bearing morpholine was found to be the most active cytotoxicagent with IC50 1.71 (MCF-7), 1.84 (SKOV3), and 1.1 mu M(PC-3) and a thymidylate synthase (TS) inhibitor with an IC50 of 0.81 mu M. Further cellular studies showed that compound 17 could induce apoptosis and arrest the cell cycle at theS phase in PC-3 carcinoma. The docking study strongly favors compound 17 to be a TS inhibitor as it displayed a similar interactionto 5-fluorouracil. The in silico pharmacokinetics and DFT computationalstudies support the results obtained from docking and biological evaluationand displayed favorable pharmacokinetic profile for a drug to be orallyavailable. Compound 17 was found to be a promising TSinhibitor which could suppress DNA synthesis and consequently DNAdamage in prostate cancer cells.
引用
收藏
页码:18811 / 18822
页数:12
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