Enhancing Antileishmanial Activity of Amidoxime-Based Compounds Bearing a 4,5-Dihydrofuran Scaffold: In Vitro Screening Against Leishmania amazonensis.

IF 4.2 2区 化学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecules Pub Date : 2024-11-20 DOI:10.3390/molecules29225469
Fabiana Maia Santos Urbancg Moncorvo, Oscar Leonardo Avendaño Leon, Christophe Curti, Youssef Kabri, Sébastien Redon, Eduardo Caio Torres-Santos, Patrice Vanelle
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Abstract

Leishmaniasis, a protozoan disease affecting humans, exposes significant shortcomings in current treatments. In continuation to our previous findings on amidoxime-based antileishmanial compounds bearing a 4,5-dihydrofuran scaffold, twelve new amidoxime derivatives substituted at position 3 with an amide bearing a nitrogen heterocycle were synthesized. This series was designed to replace the sulfone and aryl group on a previously reported HIT. The synthesis of these compounds involved the following three-step pathway: manganese (III) acetate-based cyclization of a β-ketoester, followed by amidation with LiHMDS and a final reaction with hydroxylamine. Three of them, containing either bromine, chlorine, or methyl substitutions and featuring a pyridine moiety, showed an interesting toxicity-activity relationship in vitro. They exhibited IC50 values of 15.0 µM, 16.0 µM, and 17.0 µM against the promastigote form of the parasite and IC50 values of 0.5 µM, 0.6 µM, and 0.3 µM against the intracellular amastigote form, respectively. A selectivity index (SI) greater than 300 was established between the cytotoxic concentrations (in murine macrophages) and the effective concentrations (against the intracellular form of Leishmania amazonensis). This SI is at least seventy times higher than that observed for Pentamidine and twenty-five times higher than that observed for the reference HIT, as previously reported.

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增强含有 4,5-二氢呋喃支架的脒基化合物的抗利什曼活性:针对亚马逊利什曼原虫的体外筛选。
利什曼病是一种影响人类的原生动物疾病,暴露出当前治疗方法的重大缺陷。为了延续我们之前对带有 4,5-二氢呋喃支架的脒肟类抗利什曼病化合物的研究成果,我们合成了 12 种新的脒肟衍生物,它们的第 3 位被带有氮杂环的酰胺取代。这一系列化合物的设计目的是取代以前报道过的 HIT 上的砜基和芳基。这些化合物的合成过程分为以下三步:以乙酸锰(III)为基础的 β-酮酯环化,然后用 LiHMDS 进行酰胺化,最后与羟胺反应。其中三种化合物含有溴、氯或甲基取代,并以吡啶分子为特征,在体外显示出有趣的毒性-活性关系。它们对寄生虫原生体的 IC50 值分别为 15.0 µM、16.0 µM 和 17.0 µM,对细胞内原生体的 IC50 值分别为 0.5 µM、0.6 µM 和 0.3 µM。在细胞毒性浓度(在小鼠巨噬细胞中)和有效浓度(对细胞内形式的亚马逊利什曼原虫)之间确定了大于 300 的选择性指数(SI)。这一选择性指数比先前报告的喷他脒至少高出 70 倍,比参考 HIT 高出 25 倍。
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来源期刊
Molecules
Molecules 化学-有机化学
CiteScore
7.40
自引率
8.70%
发文量
7524
审稿时长
1.4 months
期刊介绍: Molecules (ISSN 1420-3049, CODEN: MOLEFW) is an open access journal of synthetic organic chemistry and natural product chemistry. All articles are peer-reviewed and published continously upon acceptance. Molecules is published by MDPI, Basel, Switzerland. Our aim is to encourage chemists to publish as much as possible their experimental detail, particularly synthetic procedures and characterization information. There is no restriction on the length of the experimental section. In addition, availability of compound samples is published and considered as important information. Authors are encouraged to register or deposit their chemical samples through the non-profit international organization Molecular Diversity Preservation International (MDPI). Molecules has been launched in 1996 to preserve and exploit molecular diversity of both, chemical information and chemical substances.
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