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• W4386821017 endingPage "1833" @default.
• W4386821017 startingPage "1821" @default.
• W4386821017 abstract "Each year, approximately 50,000 children under 5 die as a result of diarrhea caused by Cryptosporidium parvum, a protozoan parasite. There are currently no effective drugs or vaccines available to cure or prevent Cryptosporidium infection, and there are limited tools for identifying and validating targets for drug or vaccine development. We previously reported a high throughput screening (HTS) of a large compound library against Plasmodium N-myristoyltransferase (NMT), a validated drug target in multiple protozoan parasite species. To identify molecules that could be effective against Cryptosporidium, we counter-screened hits from the Plasmodium NMT HTS against Cryptosporidium NMT. We identified two potential hit compounds and validated them against CpNMT to determine if NMT might be an attractive drug target also for Cryptosporidium. We tested the compounds against Cryptosporidium using both cell-based and NMT enzymatic assays. We then determined the crystal structure of CpNMT bound to Myristoyl-Coenzyme A (MyrCoA) and structures of ternary complexes with MyrCoA and the hit compounds to identify the ligand binding modes. The binding site architectures display different conformational states in the presence of the two inhibitors and provide a basis for rational design of selective inhibitors." @default.
• W4386821017 created "2023-09-19" @default.
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• W4386821017 date "2023-09-18" @default.
• W4386821017 modified "2023-10-15" @default.
• W4386821017 title "Identification of and Structural Insights into Hit Compounds Targeting <i>N</i>-Myristoyltransferase for <i>Cryptosporidium</i> Drug Development" @default.
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• W4386821017 doi "https://doi.org/10.1021/acsinfecdis.3c00151" @default.

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