Exploring chloro-isoxazole compounds inspired on tetrahydrofuran neolignans as promising antileishmanial agents

IF 5.9 2区医学 Q1 CHEMISTRY, MEDICINAL European Journal of Medicinal Chemistry Pub Date : 2025-03-08 DOI:10.1016/j.ejmech.2025.117478

Amarith R. das Neves , Diego B. Carvalho , Luiz F.P. Pereira , Rafael F. Rosalem , Cristiane Y.K. Shiguemoto , Rafael S. Orofino , Fernanda Silva , Gleice K.G. Silva , Erika P. Machado , Thalita B. Riul , Najla M. Kassab , Gabriela R. Hurtado , Pamella F. Castilho , Kelly M.P. Oliveira , Alda M.T. Ferreira , Eliane M. Piranda , Carla C.P. Arruda , Adriano C.M. Baroni

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Abstract

The present work aims to synthesize and to identify a potential antileishmanial agent from chloro-diphenyl isoxazole methoxylated compounds. We have synthesized ten new chloro-isoxazole analogs inspired by the scaffold of tetrahydrofuran neolignans veraguensin 1a, grandisin 1b, and machilin G 1c. To obtain analogs 4a-4j, we used a cycloaddition reaction with yields ranging from 45 % to 89 %. All compounds were characterized using Nuclear Magnetic Resonance of ¹H and ¹³C and analyzed by using High-Resolution Mass Spectrometry. The HPLC analysis confirmed that all compounds were more than 95 % pure. Finally, we tested the antileishmanial activity of these analogs against promastigote and intracellular amastigote forms of L. amazonensis in vitro. We conducted tests on murine peritoneal macrophages to determine the cytotoxicity of the analogs. Our findings revealed that 4e (R₁–R₃ = –OCH₃, X₁ = -Cl, R₄ and R₅ = –OCH₂O-), a hybrid compound of grandisin and machilin G, showed moderate activity on promastigotes (IC₅₀ = 38.1 ± 1.5 μM). 4e was also effective against intracellular amastigotes with similar IC₅₀ values to AmB-treated control (IC₅₀ = 2.2 ± 0.4 μM and IC₅₀ = 2.0 ± 0.1, respectively). Moreover, it exhibited a selectivity index (SI) for amastigote forms equal to 22.7, higher than the reference drugs we tested. Analog 4e displayed non-mutagenic potential at all tested concentrations in the Ames test. We also evaluated the therapeutic effect of 4e on the experimental cutaneous leishmaniasis model with BALB/c mice infected with promastigote forms of L. amazonensis and treated with intralesional (IL) injections. Our study found that mice treated with 4e had a significant reduction (99.5 % drop) in the footpad tissue parasite load compared to the control group treated with the vehicle. The effect of 4e was similar, controlling the infection, to that of N-methylglucamine antimonate (Sb, Glucantime, 99.8 % drop), which is a reference treatment. Based on our results, we suggest that chloro-isoxazole analog 4e shows potential as an antileishmanial agent for treating cutaneous leishmaniasis (CL).

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探索以四氢呋喃新木质素为灵感的氯代异噁唑化合物作为有前途的抗利什曼病药物

本工作旨在从氯-二苯基异恶唑甲氧基化化合物中合成并鉴定一种潜在的抗利什曼病药物。我们以四氢呋喃neolignans veraguensin 1a， grandisin 1b和machilin g1c为骨架，合成了10个新的氯异恶唑类似物。为了获得类似物4a-4j，我们使用了产率从45%到89%的环加成反应。所有化合物均采用1H和13C核磁共振进行了表征，并用高分辨率质谱进行了分析。HPLC分析证实所有化合物的纯度都在95%以上。最后，我们在离体实验中测试了这些类似物对亚马孙乳杆菌promastigote和胞内amastigote的抗利什曼原虫活性。我们对小鼠腹腔巨噬细胞进行了实验，以确定类似物的细胞毒性。结果表明，4e （R1-R3= - och3, X1= - cl， R4和R5= - och2o -）是grandisin和machilin G的杂化化合物，对promastigotes具有中等活性（IC50 = 38.1±1.5 μM）。4e对胞内无梭菌也有效，IC50值与amb处理的对照相似（IC50 = 2.2±0.4 μM和IC50 = 2.0±0.1）。此外，该试剂对无尾螺旋体的选择性指数（SI）为22.7，高于参比药物。在Ames试验中，模拟物4e在所有测试浓度下都显示出非诱变潜力。我们还评估了4e对BALB/c小鼠皮肤利什曼病模型的治疗效果，BALB/c小鼠感染了亚马逊乳杆菌的promastigote形式，并用IL注射治疗。我们的研究发现，与对照组相比，用4e治疗的小鼠足垫组织寄生虫负荷显著减少（下降99.5%）。4e在控制感染方面的效果与对照治疗n -甲基氨葡胺锑酸盐（Sb，葡聚糖酶，下降99.8%）相似。基于我们的结果，我们认为氯异恶唑类似物4e显示出治疗皮肤利什曼病（CL）的抗利什曼药物的潜力。

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来源期刊

European Journal of Medicinal Chemistry 化学-医药化学

CiteScore

11.70

自引率

9.00%

发文量

863

审稿时长

29 days

期刊介绍： The European Journal of Medicinal Chemistry is a global journal that publishes studies on all aspects of medicinal chemistry. It provides a medium for publication of original papers and also welcomes critical review papers. A typical paper would report on the organic synthesis, characterization and pharmacological evaluation of compounds. Other topics of interest are drug design, QSAR, molecular modeling, drug-receptor interactions, molecular aspects of drug metabolism, prodrug synthesis and drug targeting. The journal expects manuscripts to present the rational for a study, provide insight into the design of compounds or understanding of mechanism, or clarify the targets.