P-glycoprotein-9-mediated multidrug tolerance in Caenorhabditis elegans
Clara Blancfuney, Eva Guchen, Anne Lespine, Mélanie Alberich

TL;DR
This study shows that PGP-9 helps C. elegans tolerate multiple drugs, independent of other factors like NHR-8 or structural defects.
Contribution
The study provides the first direct evidence that PGP-9 is essential for multidrug tolerance in C. elegans, independent of NHR-8 regulation.
Findings
P-glycoprotein-9 (PGP-9) is necessary for multidrug tolerance in C. elegans.
PGP-9 operates independently of amphid structural defects and NHR-8 regulation.
RNAi targeting pgp-9 increases drug sensitivity in C. elegans.
Abstract
The active drug efflux pumps P-glycoproteins (PGPs) are the cornerstones of multidrug resistance in many organisms. In parasitic helminths, resistance to macrocyclic lactones (MLs) has been associated with pgp regulation and structural defects in amphids. In Caenorhabditis elegans, the nuclear hormone receptor (NHR)-8 also influences xenobiotic tolerance by regulating pgp genes. However, the specific contribution of individual transporters and their regulation remain poorly defined. We recently demonstrated that PGP-9 specifically contributes to ivermectin (IVM) tolerance in an IVM-resistant C. elegans strain. This study aimed to explore the role of PGP-9 in drug efflux in C. elegans. We used the IVM-resistant and dye-filling defective (Dyf) C. elegans strain IVR10 and a pgp-9 IVR10 mutant to assess larval development under MLs (eprinomectin (EPR) and moxidectin (MOX)) and tunicamycin…
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Taxonomy
TopicsGenetics, Aging, and Longevity in Model Organisms · Heat shock proteins research · Alzheimer's disease research and treatments
