Series of Alkynyl-Substituted Thienopyrimidines as Inhibitors of Protozoan Parasite Proliferation

Discovery of new chemotherapeutic lead agents can be accelerated by optimizing chemotypes proven to be effective in other diseases to act against parasites. One such medicinal chemistry campaign has focused on optimizing the anilinoquinazoline drug lapatinib (1) and the alkynyl thieno­[3,2-d]­pyrimi...

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Published inACS medicinal chemistry letters Vol. 9; no. 10; pp. 996 - 1001
Main Authors Woodring, Jennifer L, Behera, Ranjan, Sharma, Amrita, Wiedeman, Justin, Patel, Gautam, Singh, Baljinder, Guyett, Paul, Amata, Emanuele, Erath, Jessey, Roncal, Norma, Penn, Erica, Leed, Susan E, Rodriguez, Ana, Sciotti, Richard J, Mensa-Wilmot, Kojo, Pollastri, Michael P
Format Journal Article
LanguageEnglish
Published WASHINGTON American Chemical Society 11.10.2018
Amer Chemical Soc
Subjects
Chemistry, Medicinal
Letter
Life Sciences & Biomedicine
Pharmacology & Pharmacy
Science & Technology
Chagas
thienopyrimidines
Trypanosomes
human African trypanosomiasis (HAT)
leishmaniasis
malaria
protozoan parasite inhibitors
TRYPANOSOMA-BRUCEI
LEAD DISCOVERY
DISEASE DRUG DISCOVERY
LAPATINIB
TYROSINE KINASE INHIBITOR
CELL-CYCLE
OPTIMIZATION
GROWTH-FACTOR
SCAFFOLDS
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Summary:Discovery of new chemotherapeutic lead agents can be accelerated by optimizing chemotypes proven to be effective in other diseases to act against parasites. One such medicinal chemistry campaign has focused on optimizing the anilinoquinazoline drug lapatinib (1) and the alkynyl thieno­[3,2-d]­pyrimidine hit GW837016X (NEU-391, 3) into leads for antitrypanosome drugs. We now report the structure–activity relationship studies of 3 and its analogs against Trypanosoma brucei, which causes human African trypanosomiasis (HAT). The series was also tested against Trypanosoma cruzi, Leishmania major, and Plasmodium falciparum. In each case, potent antiparasitic hits with acceptable toxicity margins over mammalian HepG2 and NIH3T3 cell lines were identified. In a mouse model of HAT, 3 extended life of treated mice by 50%, compared to untreated controls. At the cellular level, 3 inhibited mitosis and cytokinesis in T. brucei. Thus, the alkynylthieno­[3,2-d]­pyrimidine chemotype is an advanced hit worthy of further optimization as a potential chemotherapeutic agent for HAT.
Bibliography:NIH RePORTER
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ISSN:1948-5875
1948-5875
DOI:10.1021/acsmedchemlett.8b00245