Screening to Identify Anti- Compounds and Modeling for Bioactivities and Toxicity

Overview

Journal Yale J Biol Med

Specialty Biology

Date 2019 Sep 24

PMID 31543702

Citations 17

Authors

Oluyomi Stephen Adeyemi

Olubunmi Atolani

Oluwakemi Josephine Awakan

Tomilola Debby Olaolu

Charles Obiora Nwonuma

Omokolade Alejolowo

David Adeiza Otohinoyi

Damilare Rotimi

Akinyomade Owolabi

Gaber El-Saber Batiha

Affiliations

Soon will be listed here.

Abstract

Toxoplasmosis, which affects more than a billion people worldwide, is a common parasitic infection caused by the obligate intracellular parasite, . Current treatment strategies have several limitations, including unwanted side effects and poor efficacy. Therefore, newer therapies are needed for toxoplasmosis. Drug repurposing and screening of a vast array of natural and/or synthetic compounds is a viable option for antiparasitic drug discovery. In this study, we screened 62 compounds comprising natural products (NPs) and FDA-approved (FDA) drugs, to identify the hit compounds that suppress the growth of . To determine the parasite inhibitory potential of the compounds, host mammalian cells were infected with a transgenic strain, and the viability of the parasite was evaluated by luminescence. Of the 62 compounds, tubericidin, sulfuretin, peruvoside, resveratrol, narasin and diacetoxyscirpenol of the natural product isolates, as well as bortezonib, 10-Hydroxycamtothecin, mebendazole, niflumic acid, clindamycin HCl, mecamylamine, chloroquine, mitomycin C, fenbendazole, daunorubicin, atropine, and cerivastatin of FDA molecules were identified as "hits" with ≥ 40 percent anti-parasite action. Additionally, mitomycin C, radicicol, naringenin, gitoxigenin, menadione, botulin, genistin, homobutein, and gelsemin HCl of the natural product isolates, as well as lomofungin, cyclocytidine, prazosin HCl, cerivastatin, camptothecin, flufenamic acid, atropine, daunorubicin, and fenbendazole of the FDA compounds exhibited cytotoxic activity, reducing the host viability by ≥ 30 percent. Our findings not only support the prospects of drug repurposing, but also indicate that screening a vast array of molecules may provide viable sources of alternative therapies for parasitic infection.

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