| Literature DB >> 34936384 |
Sang-Kyu Park1, Lukas Friedrich2, Nawal A Yahya1,3, Claudia M Rohr1, Evgeny G Chulkov1, David Maillard4, Friedrich Rippmann2, Thomas Spangenberg5, Jonathan S Marchant1.
Abstract
Praziquantel (PZQ) is an essential medicine for treating parasitic flatworm infections such as schistosomiasis, which afflicts over 250 million people. However, PZQ is not universally effective, lacking activity against liver flukes of the Fasciola genus. The reason for this insensitivity is unclear, as the mechanism of PZQ action is unknown. Here, we use ligand- and target-based methods to demonstrate that PZQ activates a transient receptor potential melastatin ion channel (TRPMPZQ) in schistosomes by engaging a hydrophobic ligand binding pocket within the voltage sensor–like domain of the channel to cause calcium entry and worm paralysis. PZQ activates TRPMPZQ homologs in other PZQ-sensitive flukes, but not Fasciola hepatica. However, a single amino acid change in the F. hepatica TRPMPZQ binding pocket, to mimic schistosome TRPMPZQ, confers PZQ sensitivity. After decades of clinical use, the molecular basis of PZQ action at a druggable TRP channel is resolved.Entities:
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Year: 2021 PMID: 34936384 PMCID: PMC8855674 DOI: 10.1126/scitranslmed.abj5832
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956