CaMKII regulates neuromuscular activity and survival of the human blood fluke Schistosoma mansoni.

Sci Rep

Molecular Parasitology Laboratory, School of Life Sciences Pharmacy and Chemistry, Kingston University, Penrhyn Road, Kingston Upon Thames, KT1 2EE, UK.

Published: November 2022

AI Article Synopsis

  • CaMKII is a vital protein that facilitates various cellular functions and is found in all life stages of the Schistosoma mansoni blood parasite, which causes schistosomiasis in humans.
  • CaMKII activation in these parasites is significantly boosted upon exposure to the anti-schistosomal drug praziquantel, leading to critical effects like reduced movement and ultimately death when CaMKII is depleted.
  • The study suggests that CaMKII interacts with numerous proteins and signaling pathways, indicating its potential as a target for developing new treatments against schistosomiasis.

Article Abstract

Calcium/calmodulin dependant protein kinase II (CaMKII), an important transducer of Ca signals, orchestrates multiple cellular functions in animals. Here we investigated the importance of CaMKII to Schistosoma mansoni, a blood parasite that causes human schistosomiasis. We demonstrate that phosphorylated (activated) CaMKII is present in cercariae, schistosomula and adult worms, and show that striking activation occurs in the nervous tissue of these parasite life-stages; CaMKII was also activated in the tegument and muscles of adult worms and the vitellaria of females. Exposure of worms to the anti-schistosomal drug praziquantel (PZQ) induced significant CaMKII activation and depletion of CaMKII protein/activation in adult worms resulted in hypokinesia, reduced vitality and death. At medium confidence (global score ≥ 0.40), S. mansoni CaMKII was predicted to interact with 51 proteins, with many containing CaMKII phosphorylation sites and nine mapped to phosphoproteome data including sites within a ryanodine receptor. The CaMKII network was functionally enriched with mitogen-activated protein kinase, Wnt, and notch pathways, and ion-transport and voltage-dependent channel protein domains. Collectively, these data highlight the intricacies of CaMKII signalling in S. mansoni, show CaMKII to be an active player in the PZQ-mediated response of schistosomes and highlight CaMKII as a possible target for the development of novel anti-schistosome therapeutics.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9674609PMC
http://dx.doi.org/10.1038/s41598-022-23962-8DOI Listing

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