A drug repurposing screen for whipworms informed by comparative genomics.

IF 3.8 2区 医学 Q1 Medicine
PLoS Neglected Tropical Diseases Pub Date : 2023-09-05 eCollection Date: 2023-09-01 DOI:10.1371/journal.pntd.0011205
Avril Coghlan, Frederick A Partridge, María Adelaida Duque-Correa, Gabriel Rinaldi, Simon Clare, Lisa Seymour, Cordelia Brandt, Tapoka T Mkandawire, Catherine McCarthy, Nancy Holroyd, Marina Nick, Anwen E Brown, Sirapat Tonitiwong, David B Sattelle, Matthew Berriman
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Abstract

Hundreds of millions of people worldwide are infected with the whipworm Trichuris trichiura. Novel treatments are urgently needed as current drugs, such as albendazole, have relatively low efficacy. We have investigated whether drugs approved for other human diseases could be repurposed as novel anti-whipworm drugs. In a previous comparative genomics analysis, we identified 409 drugs approved for human use that we predicted to target parasitic worm proteins. Here we tested these ex vivo by assessing motility of adult worms of Trichuris muris, the murine whipworm, an established model for human whipworm research. We identified 14 compounds with EC50 values of ≤50 μM against T. muris ex vivo, and selected nine for testing in vivo. However, the best worm burden reduction seen in mice was just 19%. The high number of ex vivo hits against T. muris shows that we were successful at predicting parasite proteins that could be targeted by approved drugs. In contrast, the low efficacy of these compounds in mice suggest challenges due to their chemical properties (e.g. lipophilicity, polarity, molecular weight) and pharmacokinetics (e.g. absorption, distribution, metabolism, and excretion) that may (i) promote absorption by the host gastrointestinal tract, thereby reducing availability to the worms embedded in the large intestine, and/or (ii) restrict drug uptake by the worms. This indicates that identifying structural analogues that have reduced absorption by the host, and increased uptake by worms, may be necessary for successful drug development against whipworms.

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根据比较基因组学的信息,对鞭虫进行药物再利用筛选。
全世界有数亿人感染了鞭虫鞭虫。迫切需要新的治疗方法,因为目前的药物,如阿苯达唑,疗效相对较低。我们已经调查了批准用于其他人类疾病的药物是否可以被重新用作新型抗鞭虫药物。在之前的比较基因组学分析中,我们确定了409种批准用于人类的药物,我们预测这些药物可以靶向寄生虫蛋白。在这里,我们通过评估鼠鞭虫(一种已建立的人类鞭虫研究模型)成虫的运动性来进行体外测试。我们在体外鉴定了14种对鼠尾丝虫EC50值≤50μM的化合物,并选择了9种进行体内测试。然而,在小鼠身上看到的最好的蠕虫负担减轻只有19%。对T.muris的大量离体攻击表明,我们成功地预测了可能被批准的药物靶向的寄生虫蛋白。相反,这些化合物在小鼠中的低功效表明,由于它们的化学性质(如亲脂性、极性、分子量)和药代动力学(如吸收、分布、代谢和排泄),它们可能(i)促进宿主胃肠道的吸收,从而降低包埋在大肠中的蠕虫的可用性,和/或(ii)限制蠕虫对药物的摄取。这表明,鉴定宿主吸收减少、蠕虫吸收增加的结构类似物,对于成功开发针对鞭虫的药物可能是必要的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PLoS Neglected Tropical Diseases
PLoS Neglected Tropical Diseases Medicine-Infectious Diseases
CiteScore
7.40
自引率
10.50%
发文量
723
审稿时长
2-3 weeks
期刊介绍: PLOS Neglected Tropical Diseases publishes research devoted to the pathology, epidemiology, prevention, treatment and control of the neglected tropical diseases (NTDs), as well as relevant public policy. The NTDs are defined as a group of poverty-promoting chronic infectious diseases, which primarily occur in rural areas and poor urban areas of low-income and middle-income countries. Their impact on child health and development, pregnancy, and worker productivity, as well as their stigmatizing features limit economic stability. All aspects of these diseases are considered, including: Pathogenesis Clinical features Pharmacology and treatment Diagnosis Epidemiology Vector biology Vaccinology and prevention Demographic, ecological and social determinants Public health and policy aspects (including cost-effectiveness analyses).
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