Cisplatin and Procaterol Combination in Gastric Cancer? Targeting Checkpoint Kinase 1 for Cancer Drug Discovery and Repurposing by an Integrated Computational and Experimental Approach.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-01-01 Epub Date: 2024-01-08 DOI:10.1089/omi.2023.0163
Suchitha Giridhara Prema, Jaikanth Chandrasekaran, Saptami Kanekar, Mejo George, Thottethodi Subrahmanya Keshava Prasad, Rajesh Raju, Shobha Dagamajalu, Rex Devasahayam Arokia Balaya
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Abstract

Checkpoint kinase 1 (CHK1), a serine/threonine kinase, plays a crucial role in cell cycle arrest and is a promising therapeutic target for drug development against cancers. CHK1 coordinates cell cycle checkpoints in response to DNA damage, facilitating repair of single-strand breaks, and maintains the genome integrity in response to replication stress. In this study, we employed an integrated computational and experimental approach to drug discovery and repurposing, aiming to identify a potent CHK1 inhibitor among existing drugs. An e-pharmacophore model was developed based on the three-dimensional crystal structure of the CHK1 protein in complex with CCT245737. This model, characterized by seven key molecular features, guided the screening of a library of drugs through molecular docking. The top 10% of scored ligands were further examined, with procaterol emerging as the leading candidate. Procaterol demonstrated interaction patterns with the CHK1 active site similar to CHK1 inhibitor (CCT245737), as shown by molecular dynamics analysis. Subsequent in vitro assays, including cell proliferation, colony formation, and cell cycle analysis, were conducted on gastric adenocarcinoma cells treated with procaterol, both as a monotherapy and in combination with cisplatin. Procaterol, in synergy with cisplatin, significantly inhibited cell growth, suggesting a potentiated therapeutic effect. Thus, we propose the combined application of cisplatin and procaterol as a novel potential therapeutic strategy against human gastric cancer. The findings also highlight the relevance of CHK1 kinase as a drug target for enhancing the sensitivity of cytotoxic agents in cancer.

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胃癌中的顺铂和丙卡特罗联合疗法?通过综合计算和实验方法靶向检查点激酶 1 以发现抗癌药物并进行再利用。
检查点激酶 1(CHK1)是一种丝氨酸/苏氨酸激酶,在细胞周期停滞过程中发挥着至关重要的作用,是开发抗癌药物的一个前景看好的治疗靶点。CHK1 在应对 DNA 损伤时协调细胞周期检查点,促进单链断裂的修复,并在应对复制压力时保持基因组的完整性。在这项研究中,我们采用了计算与实验相结合的方法来发现药物并进行再利用,旨在从现有药物中找出一种强效的 CHK1 抑制剂。根据 CHK1 蛋白与 CCT245737 复合物的三维晶体结构,我们建立了一个电子药性模型。该模型以七个关键分子特征为特点,通过分子对接指导筛选药物库。对得分最高的 10% 配体进行了进一步研究,普卡特罗成为主要候选药物。分子动力学分析表明,普卡特罗与 CHK1 活性位点的相互作用模式类似于 CHK1 抑制剂(CCT245737)。随后对使用普卡特罗治疗的胃腺癌细胞进行了体外试验,包括细胞增殖、集落形成和细胞周期分析,普卡特罗既可作为单一疗法,也可与顺铂联合使用。普卡特罗与顺铂协同作用时能显著抑制细胞生长,这表明普卡特罗具有增强治疗效果的作用。因此,我们建议将顺铂和普鲁卡特罗联合应用,作为一种潜在的治疗人类胃癌的新策略。研究结果还强调了 CHK1 激酶作为提高癌症细胞毒性药物敏感性的药物靶点的相关性。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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