将斑马鱼胚胎发育毒性试验（ZEDTA）与血红蛋白染色相结合，促进新型孕妇抗疟药物的研究。

IF 4.1 2区医学 Q1 PARASITOLOGY

International Journal for Parasitology: Drugs and Drug Resistance Pub Date : 2025-01-22 DOI:10.1016/j.ijpddr.2025.100582

Lucia Borrallo-Lopez , Laura Guzman , Noelia G. Romero , Anna Sampietro , Ana Mallo-Abreu , Laia Guardia-Escote , Elisabet Teixidó , Burkhard Flick , Xavier Fernàndez-Busquets , Diego Muñoz-Torrero , Marta Barenys

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引用次数: 0

摘要

背景：怀孕期间患疟疾对母亲和发育中的儿童都有很高的风险。然而，孕妇的治疗选择历来非常有限，特别是在怀孕的前三个月，由于对胚胎-胎儿发育的潜在不利影响。最近，由于啮齿动物研究的结果与现有临床数据不一致，关于这些潜在的胚胎-胎儿不良反应存在很大争议，最后，世卫组织改变了对患有无并发症恶性疟原虫疟疾的孕妇的建议，在妊娠早期使用蒿甲醚-氨苯曲明治疗。临床前和临床研究之间的差异归因于循环原始红母细胞易感窗口时间的物种差异。方法：本文提供了一种基于动物实验替代方法的工具，加速了孕妇新药的研究。我们已经调整了斑马鱼胚胎发育毒性试验，包括胚胎中的血红蛋白染色和两个时间点的致命性和畸形发育评估。选择这两个时间点包括一个独立于红细胞功能的时间点和一个依赖于红细胞功能的时间点。该方法用于检测4种已上市的抗疟药物和3种新的抗疟候选药物。结果：我们的组合试验可以正确预测几种抗疟上市药物（青蒿素、奎宁、氯喹和双氢青蒿素+去丁基甲基苯胺）的致畸和非致畸作用。此外，我们还测试了三种新的候选药物（GS-GUAN、DONE3TCl和YAT2150），它们具有新的作用机制，不同于已上市的抗疟药。结论：我们提出了一个决策树，将两个时间点的评估结果与显著红细胞消耗的信息结合起来。该决策树的目的是在药物开发过程的早期阶段确定对致畸性或红细胞消耗没有或较低危害的化合物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Combining the zebrafish embryo developmental toxicity assay (ZEDTA) with hemoglobin staining to accelerate the research of novel antimalarial drugs for pregnant women

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Combining the zebrafish embryo developmental toxicity assay (ZEDTA) with hemoglobin staining to accelerate the research of novel antimalarial drugs for pregnant women

Background

Malaria during pregnancy implies a high risk for the mother and the developing child. However, the therapeutic options for pregnant women have historically been very limited, especially during the first trimester of pregnancy due to potential adverse effects on embryo-fetal development. Recently, there has been great controversy regarding these potential embryo-fetal adverse effects because the results of rodent studies were not in accordance with the clinical data available, and finally the WHO has changed the recommendations for pregnant women with uncomplicated P. falciparum malaria to treatment with artemether-lumefantrine during the first trimester. The discrepancy between pre-clinical and clinical studies has been attributed to species-differences in the duration of the window of susceptibility of circulating primitive erythroblasts.

Methods

Here we provide a tool based on an alternative method to animal experimentation that accelerates the research of novel drugs for pregnant women. We have adapted the zebrafish embryo developmental toxicity assay to include hemoglobin staining in the embryos and two time-points of lethality and dysmorphogenesis evaluation. These two time-points were selected to include one when the development is independent of and one when the development is dependent of erythrocytes function. The method was used to test four marketed antimalarial drugs and three new antimalarial drug candidates.

Results

Our combination of tests can correctly predict the teratogenic and non-teratogenic effects of several antimalarial marketed drugs (artemisinin, quinine, chloroquine, and dihydroartemisinin + desbutyl-lumefantrine). Furthermore, we have tested three new drug candidates (GS-GUAN, DONE3TCl, and YAT2150) with novel mechanisms of action, and different from those of the marketed antimalarial drugs.

Conclusions

We propose a decision tree combining the results of the two time-points of evaluation together with the information on significant erythrocyte depletion. The aim of this decision tree is to identify compounds with no or lower hazard on teratogenicity or erythrocyte depletion at an early phase of the drug development process.

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来源期刊

International Journal for Parasitology: Drugs and Drug Resistance PARASITOLOGY-PHARMACOLOGY & PHARMACY

CiteScore

7.90

自引率

7.50%

发文量

审稿时长

48 days

期刊介绍： The International Journal for Parasitology – Drugs and Drug Resistance is one of a series of specialist, open access journals launched by the International Journal for Parasitology. It publishes the results of original research in the area of anti-parasite drug identification, development and evaluation, and parasite drug resistance. The journal also covers research into natural products as anti-parasitic agents, and bioactive parasite products. Studies can be aimed at unicellular or multicellular parasites of human or veterinary importance.