Buxton SK , Charvet CL , Neveu C , Cabaret J , Cortet J , Peineau N , Abongwa M , Courtot E , Robertson AP , Martin RJ .

R01AI047194 NIAID NIH HHS , R21AI092185-01A1 NIAID NIH HHS , R01 AI047194 NIAID NIH HHS , R21 AI092185 NIAID NIH HHS

	Figure 2. Voltage-clamp of oocytes injected with O. dentatum Ode-unc-29 and Ode-unc-63 nAChR subunits.(A) Diagram of possible subunit arrangements of Ode-unc-29 and Ode-unc-63. X represents either UNC-63 or UNC-29 subunit. PyR, pyrantel; Tbd, tribendimidine, ACh, acetylcholine; Nic, nicotine; Bep, bephenium; The, thenium. (B) Representative traces showing the inward currents in oocytes injected with 1∶1 Ode-unc-29 and Ode-unc-63. (C) Bar chart (mean ± se) of agonists-elicited currents in the Ode-(29 - 63) Pyr-nAChR, (paired t-test, **p<0.01, ***p<0.001). All agonist responses have been normalized to the average 100 µM ACh currents. (D) Dose-response relationships for Pyr (inverted Δ, n = 6), Tbd (▴, n = 5) and ACh (•, n = 6) in the Ode-(29 - 63) Pyr-nAChR, (n = number of oocytes). (E) Bar chart (mean ± se) of normalized currents elicited by different agonists in 1∶5 Ode-unc-29∶Ode-unc-63 injected oocytes. Currents have been normalized to and compared with 100 µM ACh currents (paired t-test, **p<0.01, ***p<0.001). (F) Bar chart (mean ± se) of normalized currents elicited by different agonists in oocytes injected with 5∶1 Ode-unc-29∶Ode-unc-63. Currents normalized to and compared with 100 µM ACh currents (paired t-test, *p<0.05, **p<0.01).
	Figure 4. Effects of derquantel on levamisole-activated and pyrantel-activated expressed Ode(29-63-8-38), the Lev-nAChR, and on pyrantel-activated and levamisole-activated Ode(29-63-38), the PyR/Trbd-nAChR subtypes.Der: derquantel; Lev: levamisole; Pyr: pyrantel. (A) Antagonistic effects of varying derquantel concentrations on levamisole currents of Ode(29-63-8-38). Levamisole evokes supramaximal normalized currents and derquantel competitively inhibited levamisole currents. (B) Derquantel antagonism of pyrantel currents of Ode(29-63-8-38). Here, derquantel produced mixed non-competitively competitive antagonism. Pyrantel did not activate supramaximal currents. (C) Antagonism of pyrantel by derquantel on the Ode(29-63-38), Pyr/Tbd-nAChR. Derquantel is a potent non-competitive antagonist. (D) Derquantel non-competitively antagonized levamisole responses on the Ode(29-63-38) receptor.
	Figure 5. Ca2+ permeability of the O. dentatum receptor subtypes with large ACh currents.(A) Current-Voltage plot for oocytes injected with Ode(29–63–8), showing the change in current with voltage in 1 mM and 10 mM Ca2+ recording solutions. Insert: Magnified view of current-voltage plot from −20 mV to +40 mV showing the Erev in 1 mM and 10 mM extracellular Ca2+. (B) Current-Voltage plot for oocytes injected with Ode(29–63–38) showing the current changes in 1 mM and 10 mM Ca2+ recording solution under different voltages. Insert: Magnified view of current-voltage plot from −20 mV to +40 mV showing the Erev in 1 mM and 10 mM extracellular Ca2+. (C) Current-Voltage plot for oocytes injected with Ode(29–63–38–8) in 1 mM and 10 mM Ca2+ recording solutions. Insert: Magnified view of current-voltage plot from −20 mV to +40 mV showing the Erev in 1 mM and 10 mM extracellular Ca2+. The calcium permeability was calculated using the GHK equation (Text S1 Legend).
	Figure 6. Single-channel properties of the Lev-nAChR subtype.(A) Representative current-voltage plot from oocyte-attached patch with 10 µM levamisole. Inserts are representative channel openings at +75 mV and −75 mV membrane potentials. Even with 10 µM levamisole, we sometimes observed ‘flickering’ channel block events; note the ‘flickering’ channel block shown by openings at −75 mV. (B) Bar chart (mean ± se) of the mean open times (τ) at the different patch potentials. (C) Bar chart (mean ± se) of the probability of channel opening, Po, at the different patch potentials.
	Figure 1. Maximum likelihood tree showing relationships of acetylcholine receptor (nAChR) subunit cDNA sequences in Oesophagostomum dentatum (Ode, highlighted in red), Caenorhabditis elegans (Cel), Haemonchus contortus (Hco) and Teladorsagia circumcincta (Tci).The C. elegans acr-16 nAChR subunit sequence was used as an outgroup. Branch support was evaluated using the chi2 option of PhyML and values more than 0.9 were considered reliable.

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