Scientific Reports (Mar 2023)

Repertoire of P-glycoprotein drug transporters in the zoonotic nematode Toxocara canis

  • Jeba R. J. Jesudoss Chelladurai,
  • Katy A. Martin,
  • Pam Vardaxis,
  • Craig Reinemeyer,
  • Paramasivan Vijayapalani,
  • Alan P. Robertson,
  • Matthew T. Brewer

DOI
https://doi.org/10.1038/s41598-023-31556-1
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 11

Abstract

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Abstract Toxocara canis has a complex lifecycle including larval stages in the somatic tissue of dogs that tolerate macrocyclic lactones. In this study, we investigated T. canis permeability glycoproteins (P-gps, ABCB1) with a putative role in drug tolerance. Motility experiments demonstrated that while ivermectin failed to abrogate larval movement, the combination of ivermectin and the P-gp inhibitor verapamil induced larval paralysis. Whole organism assays revealed functional P-gp activity in larvae which were capable of effluxing the P-gp substrate Hoechst 33342 (H33342). Further investigation of H33342 efflux demonstrated a unique rank order of potency for known mammalian P-gp inhibitors, suggesting that one or more of the T. canis transporters has nematode-specific pharmacological properties. Analysis of the T. canis draft genome resulted in the identification of 13 annotated P-gp genes, enabling revision of predicted gene names and identification of putative paralogs. Quantitative PCR was used to measure P-gp mRNA expression in adult worms, hatched larvae, and somatic larvae. At least 10 of the predicted genes were expressed in adults and hatched larvae, and at least 8 were expressed in somatic larvae. However, treatment of larvae with macrocyclic lactones failed to significantly increase P-gp expression as measured by qPCR. Further studies are needed to understand the role of individual P-gps with possible contributions to macrocyclic lactone tolerance in T. canis.