Evaluation of the antiplasmodial efficacy of synthetic 2,5-diphenyloxazole analogs of compounds naturally derived from Oxytropis lanata

Nanang R. Ariefta , Koichi Narita , Toshihiro Murata , Yoshifumi Nishikawa
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Abstract

The persistent prevalence and dissemination of drug-resistant malaria parasites continue to challenge the progress of malaria eradication efforts. As a result, there is an urgent need to search for and develop innovative therapies. In this study, we screened synthetic 2,5-diphenyloxazole analogs from Oxytropis lanata. Among 48 compounds, 14 potently inhibited the proliferation of P. falciparum strains 3D7 (chloroquine-sensitive) and K1 (multidrug-resistant) in vitro, exhibited IC50 values from 3.38 to 12.65 μM and 1.27–6.19 μM, respectively, and were toxic to human foreskin fibroblasts at 39.53–336.35 μM. Notably, Compounds 31 (2-(2′,3′-dimethoxyphenyl)-5-(2″-hydroxyphenyl)oxazole) and 32 (2-(2′,3′-dimethoxyphenyl)-5-(2″-benzyloxyphenyl)oxazole) exhibited the highest selectivity indices (SIs) against both P. falciparum strains (3D7/K1), with values > 40.20/>126.58 and > 41.27/> 59.06, respectively. In the IC50 speed and stage-specific assays, Compounds 31 and 32 showed slow action, along with distinct effects on the ring and trophozoite stages. Microscopy observations further revealed that both compounds impact the development and delay the progression of the trophozoite and schizont stages in P. falciparum 3D7, especially at concentrations 100 times their IC50 values. In a 72-h in vitro exposure experiment at their respective IC80 in P. falciparum 3D7, significant alterations in parasitemia levels were observed compared to the untreated group. In Compound 31-treated cultures, parasites shrank and were unable to reinvade red blood cells (RBCs) during an extended 144-h incubation period, even after compound removal from the culture. In vivo assessments were conducted on P. yoelii 17XNL-infected mice treated with Compounds 31 and 32 at 20 mg/kg administered once daily for ten days. The treated groups showed statistically significant lower peaks of parasitemia (Compound 31-treated: trial 1 12.7%, trial 2 15.8%; Compound 32-treated: trial 1 12.7%, trial 2 14.0%) compared to the untreated group (trial 1 21.7%, trial 2 28.3%). These results emphasize the potential of further developing 2,5-diphenyloxazoles as promising antimalarial agents.

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评估天然提取自Oxytropis lanata的化合物的合成2,5-二苯基恶唑类似物的抗疟功效
抗药性疟疾寄生虫的持续流行和传播继续对根除疟疾工作的进展构成挑战。因此,迫切需要寻找和开发创新疗法。在这项研究中,我们筛选了从Oxytropis lanata中合成的2,5-二苯基恶唑类似物。在 48 个化合物中,14 个化合物能有效抑制恶性疟原虫菌株 3D7 (氯喹敏感)和 K1 (耐多种药物)在体外的增殖,其 IC50 值分别为 3.38 至 12.65 μM 和 1.27-6.19 μM,对人包皮成纤维细胞的毒性为 39.53-336.35 μM。值得注意的是,化合物 31(2-(2′,3′-二甲氧基苯基)-5-(2″-羟基苯基)噁唑)和 32(2-(2′,3′-二甲氧基苯基)-5-(2″-苄氧基苯基)噁唑)对两种恶性疟原虫菌株(P. falciparum 和 P. falciparum)都表现出最高的选择性指数(SIs)。恶性疟原虫菌株(3D7/K1)的选择性指数(SI)最高,分别为 40.20/>126.58 和 41.27/>59.06。在 IC50 速度和阶段特异性试验中,化合物 31 和 32 显示出缓慢的作用,同时对环阶段和滋养体阶段有明显的影响。显微镜观察进一步表明,这两种化合物都会影响恶性疟原虫 3D7 滋养体和裂殖体阶段的发育并延缓其进程,尤其是在浓度为其 IC50 值 100 倍时。在恶性疟原虫 3D7 体外暴露 72 小时的实验中,在各自的 IC80 浓度下,与未处理组相比,寄生虫血症水平发生了显著变化。在经化合物 31 处理的培养物中,寄生虫在延长的 144 小时培养期内缩小,甚至在从培养物中移除化合物后也无法再侵入红细胞(RBC)。用化合物 31 和 32 对感染了 P. yoelii 17XNL 的小鼠进行了体内评估,剂量为 20 毫克/千克,每天一次,连续十天。与未处理组(试验 1 21.7%,试验 2 28.3%)相比,处理组的寄生虫血症峰值明显降低(化合物 31 处理组:试验 1 12.7%,试验 2 15.8%;化合物 32 处理组:试验 1 12.7%,试验 2 14.0%)。这些结果凸显了进一步开发 2,5-二苯基恶唑类抗疟药物的潜力。
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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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