Evaluation of Diarylureas for Activity Against <i>Plasmodium falciparum</i>

Zhang, Yiqun; Anderson, Marc O.; Weisman, Jennifer L.; Lu, Min; Choy, Cindy J.; Boyd, Vincent A.; Price, Jeanine E.; Sigal, Martina; Clark, Julie; Connelly, Michele; Zhu, Fangyi; Guiguemde, W. Armand; Jeffries, Cynthia; Yang, Lei; Lemoff, Andrew; Liou, Ally P.; Webb, Thomas R.; DeRisi, Joseph L.; Guy, R. Kiplin

doi:10.1021/ml100083c

Cited by 43 publications

(34 citation statements)

References 18 publications

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“…MMV006901 ( 597 ) is currently unreported for antimalarial activity; however, Kiplin and co‐workers identified a series of diaryl ureas (e.g., 598 ) as a promising new class of antimalarials . MMV688283 ( 33 ), discussed above, featured in the kinetoplastid category of the Pathogen Box, but was reported as an antimalarial, albeit with similar compounds being reported as kinetoplastid inhibitors .…”

Section: Malariamentioning

confidence: 99%

Unpacking the Pathogen Box—An Open Source Tool for Fighting Neglected Tropical Disease

Veale

2019

ChemMedChem

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The Pathogen Box is a 400‐strong collection of drug‐like compounds, selected for their potential against several of the world's most important neglected tropical diseases, including trypanosomiasis, leishmaniasis, cryptosporidiosis, toxoplasmosis, filariasis, schistosomiasis, dengue virus and trichuriasis, in addition to malaria and tuberculosis. This library represents an ensemble of numerous successful drug discovery programmes from around the globe, aimed at providing a powerful resource to stimulate open source drug discovery for diseases threatening the most vulnerable communities in the world. This review seeks to provide an in‐depth analysis of the literature pertaining to the compounds in the Pathogen Box, including structure–activity relationship highlights, mechanisms of action, related compounds with reported activity against different diseases, and, where appropriate, discussion on the known and putative targets of compounds, thereby providing context and increasing the accessibility of the Pathogen Box to the drug discovery community.

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Section: Malariamentioning

confidence: 99%

Unpacking the Pathogen Box—An Open Source Tool for Fighting Neglected Tropical Disease

Veale

2019

ChemMedChem

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“…The pharmacophore differs from that constructed by Zhang et al which contained 2-3 hydrophobic features and 2-3 hydrogen bond acceptors. 25 Not surprisingly, the 3 most active diaryl ureas from the paper by Zhang et al failed to map to our pharmacophore; most likely, the 4-aminoquinaldine-derived diaryl ureas present different features than the triclosan-derived diaryl ureas. Distinctions in the arrangement of hydrophobic and hydrogen bonding features in the diaryl ureas from Zhang et al and in this study may enable these molecules to target different proteins in Plasmodium falciparum.…”

mentioning

confidence: 77%

“…4 We also reported in 2005 the preparation of triclosan-based 4'-ureas (Supplementary Data Figure S1) that were less potent against cultured parasite (EC 50 values of ~100 μM) than 12 -25, but exhibited IC 50 values of ~100 nM against purified PfFabI assayed in vitro. 14 More generally, the diaryl urea class of small molecules has been previously reported in the literature to exhibit potent efficacy against cultured parasites [21][22][23][24][25] but without definitive biological target identification. This chemotype was also found amongst hits against P. falciparum dihydroorotate dehydrogenase 26 that lacked whole-cell activity.…”

mentioning

confidence: 99%

Novel diaryl ureas with efficacy in a mouse model of malaria

Anderson¹,

Sarantakis²,

Terpinski³

et al. 2013

Bioorganic & Medicinal Chemistry Letters

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“…9 In recent years, great efforts have been paid to the development of phosgenefree approaches to these compounds. For example, triphosgene, 9-11 chloroformate, 12,13 and N,N'-carbonyldiimidazole (CDI) 14 have been developed as the substitutes for phosgene. However, low atom economy limits the utility of these approaches.…”

Section: Introductionmentioning

confidence: 99%

Phosgene-free synthesis of N-aryl-N'-4-pyridinylureas via selenium-catalyzed oxidative carbonylation of 4-aminopyridine with aromatic amines

Zhang¹,

Li²,

Wang³

et al. 2016

Arkivoc

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A facile, phosgene-free approach with high atom economy has been developed for the synthesis of N-aryl-N′-(4-pyridinyl)ureas. With cheap selenium as the catalyst, carbon monoxide (instead of phosgene) as the carbonyl reagent, N-aryl-N′-(4-pyridinyl)ureas can be obtained in a one-pot manner mostly in moderate to good yields via oxidative cross-carbonylation of 4-aminopyridine with a variety of aromatic amines in the presence of oxygen under atmospheric pressure. The mechanism for the synthesis of N-aryl-N′-(4-pyridinyl)ureas is also proposed.

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Evaluation of Diarylureas for Activity Against Plasmodium falciparum

Cited by 43 publications

References 18 publications

Unpacking the Pathogen Box—An Open Source Tool for Fighting Neglected Tropical Disease

Unpacking the Pathogen Box—An Open Source Tool for Fighting Neglected Tropical Disease

Novel diaryl ureas with efficacy in a mouse model of malaria

Phosgene-free synthesis of N-aryl-N'-4-pyridinylureas via selenium-catalyzed oxidative carbonylation of 4-aminopyridine with aromatic amines

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