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- W4306761582 abstract "Abstract Current malaria treatments are threatened by drug resistance and new drugs are urgently needed. In a phenotypic screen for new antimalarials, we identified ( S )-SW228703 (( S )-SW703), a tyrosine amide with asexual blood and liver stage activity and a fast-killing profile. Resistance to ( S )-SW703 is associated with mutations in Plasmodium falciparum cyclic amine resistance locus ( Pf CARL) and P. falciparum acetyl CoA transporter ( Pf ACT), similarly to several other compounds that share features such as fast activity and liver-stage activity. Compounds with these resistance mechanisms are thought to act in the ER, though their target(s) are unknown. The tyramine of ( S )-SW703 is shared with some reported Pf CARL-associated compounds; however, we observed that strict S-stereochemistry was required for activity of ( S )-SW703, suggesting differences in mechanism of action or binding mode. ( S )-SW703 provides a new chemical series with broad activity on multiple life-cycle stages and a fast-killing mechanism of action, available for lead optimization to generate new treatments for malaria." @default.
- W4306761582 created "2022-10-19" @default.
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- W4306761582 date "2022-10-17" @default.
- W4306761582 modified "2023-10-17" @default.
- W4306761582 title "A fast-killing tyrosine amide ((<i>S</i>)-SW228703) with blood and liver-stage antimalarial activity associated with the Cyclic Amine Resistance Locus (<i>Pf</i>CARL)" @default.
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- W4306761582 doi "https://doi.org/10.1101/2022.10.16.512381" @default.
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