Identification of Inhibitors of the Schistosoma mansoni VKR2 Kinase Domain.
Indran MathavanLawrence J LiuSean W RobinsonNelly El-SakkaryAdam Jo J ElaticoDarwin GomezRicky NellasRaymond J OwensWilliam J ZuercherIva Hopkins NavratilovaConor R CaffreyKonstantinos BeisPublished in: ACS medicinal chemistry letters (2022)
Schistosomiasis is a neglected tropical disease caused by parasitic flatworms. Current treatment relies on just one partially effective drug, praziquantel (PZQ). Schistosoma mansoni Venus Kinase Receptors 1 and 2 (SmVKR1 and SmVKR2) are important for parasite growth and egg production, and are potential targets for combating schistosomiasis. VKRs consist of an extracellular Venus Flytrap Module (VFTM) linked via a transmembrane helix to a kinase domain. Here, we initiated a drug discovery effort to inhibit the activity of the SmVKR2 kinase domain (SmVKR2 KD ) by screening the GSK published kinase inhibitor set 2 (PKIS2). We identified several inhibitors, of which four were able to inhibit its enzymatic activity and induced phenotypic changes in ex vivo S. mansoni . Our crystal structure of the SmVKR2 KD displays an active-like state that sheds light on the activation process of VKRs. Our data provide a basis for the further exploration of SmVKR2 as a possible drug target.
Keyphrases
- drug discovery
- protein kinase
- tyrosine kinase
- climate change
- emergency department
- drug induced
- signaling pathway
- electronic health record
- hydrogen peroxide
- nitric oxide
- randomized controlled trial
- oxidative stress
- systematic review
- combination therapy
- deep learning
- human health
- cell proliferation
- dna binding
- data analysis