Robenidine derivatives as potential antischistosomal drug candidates

IF 4.1 2区 医学 Q1 PARASITOLOGY
Christian N. Lotz , Alina Krollenbrock , Lea Imhof , Michael Riscoe , Jennifer Keiser
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引用次数: 0

Abstract

Schistosomiasis caused by Schistosoma spp. is a disease that causes a considerable health burden to millions of people worldwide. The limited availability of effective drugs on the market and the increased risk of resistance development due to extensive usage, highlight the urgent need for new antischistosomal drugs. Recent studies have shown that robenidine derivatives, containing an aminoguanidine core, exhibit promising activities against Plasmodium falciparum, motivating further investigation into their efficacy against Schistosoma mansoni, due to their similar habitat and the resulting related cellular mechanisms like the heme detoxification pathway. The conducted phenotypic screening of robenidine and 80 derivatives against newly transformed schistosomula and adult Schistosoma mansoni yielded 11 candidates with low EC50 values for newly transformed schistosomula (1.12–4.63 μM) and adults (2.78–9.47 μM). The structure-activity relationship revealed that electron-withdrawing groups at the phenyl moiety, as well as the presence of methyl groups adjacent to the guanidine moiety, enhanced the activity of derivatives against both stages of Schistosoma mansoni. The two compounds 2,2′-Bis[(3-cyano-4-fluorophenyl)methylene] carbonimidic Dihydrazide Hydrochloride (1) and 2,2′-Bis[(4-difluoromethoxyphenyl) ethylidene] carbonimidic Dihydrazide Hydrochloride (19), were selected for an in vivo study in Schistosoma mansoni-infected mice based on their potency, cytotoxicity, pharmacokinetic-, and physicochemical properties, but failed to reduce the worm burden significantly (worm burden reduction <20%). Thus, robenidine derivatives require further refinements to obtain higher antischistosomal specificity and in vivo activity.

Abstract Image

罗贝尼丁衍生物作为潜在的抗异染色体药物候选物
由血吸虫引起的血吸虫病给全世界数百万人的健康造成了巨大负担。市场上有效药物有限,而广泛使用又增加了产生抗药性的风险,因此迫切需要新的抗血吸虫药物。最近的研究表明,含有氨基胍内核的知更鸟苷衍生物对恶性疟原虫表现出良好的活性,这促使人们进一步研究它们对曼氏血吸虫的疗效,因为它们的习性相似,并由此产生了相关的细胞机制,如血红素解毒途径。对新转化血吸虫和曼氏血吸虫成虫进行的罗贝尼定及其 80 种衍生物表型筛选得出了 11 种候选药物,它们对新转化血吸虫(1.12-4.63 μM)和成虫(2.78-9.47 μM)的 EC50 值较低。结构-活性关系显示,苯基上的抽电子基团以及胍基旁甲基的存在增强了衍生物对曼氏血吸虫两个阶段的活性。2,2′-Bis[(3-cyano-4-fluorophenyl)methylene] carbonimidic Dihydrazide Hydrodrochloride (1) 和 2,2′-Bis[(4-difluoromethoxyphenyl)ethylidene] carbonimidic Dihydrazide Hydrochloride (19) 这两种化合物被选中进行体内试验、根据其药效、细胞毒性、药动学和理化特性,这些药物被选中用于曼氏血吸虫感染小鼠的体内研究,但未能显著减少虫体负荷(虫体负荷减少 <;20%).因此,知更鸟苷衍生物需要进一步改进,以获得更高的抗异吸虫特异性和体内活性。
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来源期刊
CiteScore
7.90
自引率
7.50%
发文量
31
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.
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