Evaluation of 1,10-phenanthroline-based hydroxamate derivative as dual histone deacetylases/ribonucleotide reductase inhibitor with antitumor activities

IF 2.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY
Manasa Gangadhar Shetty, Padmini Pai, Bipasa Dey, Kapaettu Satyamoorthy, Suranjan Shil, Usha Yogendra Nayak, Ashwini T, Babitha Kampa Sundara
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Abstract

Background

Aberrant expression of histone deacetylases (HDACs) and ribonucleotide reductase (RR) enzymes are commonly observed in various cancers. Researchers are focusing on these enzymes in cancer studies with the aim of developing effective chemotherapeutic drugs for cancer treatment. Targeting both HDAC and RR simultaneously with a dual HDAC/RR inhibitor has exhibited enhanced effectiveness compared to monotherapy in cancer treatment, making it a promising strategy.

Objectives

The objective of the study is to synthesize and assess the anti-cancer properties of a 1,10-phenanthroline-based hydroxamate derivative, characterizing it as a novel dual HDAC/RR inhibitor.

Methods

The N1-hydroxy-N8-(1,10-phenanthrolin-5-yl)octanediamide (PA), a 1,10-phenanthroline-based hydroxamate derivative, was synthesized and structurally characterized. The compound was subjected to in vitro assessments of its anti-cancer, HDAC, and RR inhibitory activities. In silico docking and molecular dynamics simulations were further studied to explore its interactions with HDACs and RRM2.

Results

The structurally confirmed PA exhibited antiproliferative activity in SiHa cells with an IC50 of 16.43 μM. It displayed potent inhibitory activity against HDAC and RR with IC50 values of 10.80 μM and 9.34 μM, respectively. Co-inhibition of HDAC and RR resulted in apoptosis-induced cell death in SiHa cells, mediated by the accumulation of reactive oxygen species (ROS). In silico docking studies demonstrated that PA can effectively bind to the active sites of HDAC isoforms and RRM2. Furthermore, PA demonstrated a more favorable interaction with HDAC7, displaying a docking score of -9.633 kcal/mol, as compared to the standard HDAC inhibitor suberoylanilide hydroxamic acid (SAHA), which exhibited a docking score of -8.244 kcal/mol against HDAC7.

Conclusion

The present study emphasizes the prospect of designing a potential 1,10-phenanthroline hydroxamic acid derivative as a novel dual HDAC and RR-inhibiting anti-cancer molecule.

Graphical Abstract

Abstract Image

评估 1,10-菲罗啉基羟酰胺衍生物作为组蛋白去乙酰化酶/核糖核苷酸还原酶双重抑制剂的抗肿瘤活性
背景组蛋白去乙酰化酶(HDAC)和核糖核苷酸还原酶(RR)的大量表达常见于各种癌症。研究人员在癌症研究中重点关注这些酶,以期开发出有效的化疗药物来治疗癌症。与单一疗法相比,同时以 HDAC 和 RR 为靶点的 HDAC/RR 双重抑制剂在癌症治疗中显示出更强的有效性,因此是一种很有前景的策略。本研究的目的是合成并评估一种 1,10- 菲罗啉基羟酰胺衍生物的抗癌特性,将其表征为一种新型 HDAC/RR 双重抑制剂。方法合成了一种 1,10- 菲罗啉基羟酰胺衍生物 N1-hydroxy-N8-(1,10--phenanthrolin-5-yl)octanediamide (PA),并对其进行了结构表征。对该化合物的抗癌、HDAC 和 RR 抑制活性进行了体外评估。结果经结构确认的 PA 在 SiHa 细胞中具有抗增殖活性,IC50 为 16.43 μM。它对 HDAC 和 RR 具有很强的抑制活性,IC50 值分别为 10.80 μM 和 9.34 μM。在活性氧(ROS)积累的介导下,HDAC和RR的联合抑制导致了SiHa细胞凋亡诱导的细胞死亡。硅学对接研究表明,PA 能有效地与 HDAC 异构体和 RRM2 的活性位点结合。此外,与标准 HDAC 抑制剂亚伯酰苯胺羟肟酸(SAHA)相比,PA 与 HDAC7 的相互作用更为有利,其对接得分为 -9.633 kcal/mol,而后者与 HDAC7 的对接得分为 -8.244 kcal/mol。
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来源期刊
DARU Journal of Pharmaceutical Sciences
DARU Journal of Pharmaceutical Sciences PHARMACOLOGY & PHARMACY-
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期刊介绍: DARU Journal of Pharmaceutical Sciences is a peer-reviewed journal published on behalf of Tehran University of Medical Sciences. The journal encompasses all fields of the pharmaceutical sciences and presents timely research on all areas of drug conception, design, manufacture, classification and assessment. The term DARU is derived from the Persian name meaning drug or medicine. This journal is a unique platform to improve the knowledge of researchers and scientists by publishing novel articles including basic and clinical investigations from members of the global scientific community in the forms of original articles, systematic or narrative reviews, meta-analyses, letters, and short communications.
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