Eslam B Elkaeed, Walid E Elgammal, Hazem Elkady, Hazem A Mahdy, Aisha A Alsfouk, Dalal Z Husein, Omar A Soliman, Mariam Omara, Ibrahim H Eissa, Ahmed M Metwaly
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Computational studies confirmed stable binding at VEGFR-2 active sites.</p><p><strong>Conclusion: </strong>Compound 11a is a promising thiadiazole-based candidate with notable in vitro potency, selectivity, and mechanistic activity, supporting its potential for further pharmacokinetics/toxicity evaluation and structural refinement as a VEGFR-2-targeted agent.</p>","PeriodicalId":12475,"journal":{"name":"Future medicinal chemistry","volume":" ","pages":"2145-2162"},"PeriodicalIF":3.4000,"publicationDate":"2025-09-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Discovery of new thiadiazole-based VEGFR-2 inhibitors: design, synthesis, cytotoxicity, and apoptosis induction.\",\"authors\":\"Eslam B Elkaeed, Walid E Elgammal, Hazem Elkady, Hazem A Mahdy, Aisha A Alsfouk, Dalal Z Husein, Omar A Soliman, Mariam Omara, Ibrahim H Eissa, Ahmed M Metwaly\",\"doi\":\"10.1080/17568919.2025.2552639\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>Vascular endothelial growth factor receptor-2 (VEGFR-2) is a validated target in cancer therapy. 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引用次数: 0
摘要
背景:血管内皮生长因子受体-2 (VEGFR-2)是一种有效的肿瘤治疗靶点。然而,批准的抑制剂如索拉非尼往往受到脱靶毒性和耐药性的限制。本研究旨在开发基于噻二唑的新型VEGFR-2抑制剂,具有更高的选择性和更安全的特性。方法:合理设计、合成一系列2,3-二氢-1,3,4-噻二唑衍生物,并对其进行结构表征。对MCF-7、HepG-2、HCT-116和正常WI-38细胞进行体外细胞毒性评估。机制分析包括流式细胞术检测细胞周期和凋亡,ELISA检测caspase-3、Bcl-2和Bax的表达。分子对接、200-ns分子动力学(MD)模拟、密度泛函数理论(DFT)计算和硅毒性分析支持了实验结果。结果:化合物11a表现出最有效的选择性活性(IC₅₀:MCF-7为9.49µM, HepG-2为12.89µM; SI > 3)。诱导bbb70 %的细胞凋亡和双期(S和G2/M)细胞周期阻滞。VEGFR-2抑制作用(IC₅₀= 0.055µM)与索拉非尼相当。计算研究证实VEGFR-2活性位点的稳定结合。结论:化合物11a是一种有前景的噻二唑类候选药物,具有显著的体外效力、选择性和机制活性,支持其作为vegfr -2靶向药物进行进一步的药代动力学/毒性评估和结构优化的潜力。
Discovery of new thiadiazole-based VEGFR-2 inhibitors: design, synthesis, cytotoxicity, and apoptosis induction.
Background: Vascular endothelial growth factor receptor-2 (VEGFR-2) is a validated target in cancer therapy. However, approved inhibitors like sorafenib are often limited by off-target toxicity and resistance. This study aimed to develop novel thiadiazole-based VEGFR-2 inhibitors with improved selectivity and safer profiles.
Methods: A series of 2,3-dihydro-1,3,4-thiadiazole derivatives was rationally designed, synthesized, and structurally characterized. In vitro cytotoxicity was assessed against MCF-7, HepG-2, HCT-116, and normal WI-38 cells. Mechanistic assays included flow cytometry for cell cycle and apoptosis, and ELISA for caspase-3, Bcl-2, and Bax expression. Molecular docking, 200-ns molecular dynamics (MD) simulations, density functional theory (DFT) calculations, and in silico toxicity profiling supported experimental findings.
Results: Compound 11a exhibited the most potent and selective activity (IC₅₀: 9.49 µM for MCF-7, 12.89 µM for HepG-2; SI > 3). It induced >70% apoptosis and dual-phase (S and G2/M) cell cycle arrest. VEGFR-2 inhibition (IC₅₀ = 0.055 µM) was comparable to sorafenib. Computational studies confirmed stable binding at VEGFR-2 active sites.
Conclusion: Compound 11a is a promising thiadiazole-based candidate with notable in vitro potency, selectivity, and mechanistic activity, supporting its potential for further pharmacokinetics/toxicity evaluation and structural refinement as a VEGFR-2-targeted agent.
期刊介绍:
Future Medicinal Chemistry offers a forum for the rapid publication of original research and critical reviews of the latest milestones in the field. Strong emphasis is placed on ensuring that the journal stimulates awareness of issues that are anticipated to play an increasingly central role in influencing the future direction of pharmaceutical chemistry. Where relevant, contributions are also actively encouraged on areas as diverse as biotechnology, enzymology, green chemistry, genomics, immunology, materials science, neglected diseases and orphan drugs, pharmacogenomics, proteomics and toxicology.
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