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. 2018 Apr 18;12(4):e0006420. doi: 10.1371/journal.pntd.0006420

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© 2018 Gunaratne et al

This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

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Fig 7 — (A-C) Responses to the TRPM8 agonists (A) menthol (300μM), (B) icilin (50μM) and (C) WS-12 (50μM) in wild type (WT, black) and TRPM8 knockout mice (TRPM8 KO, purple) when applied during the sustained phase of a KPSS-evoked contraction (shown by black circle). (D) Similar assay for (S)-PZQ (50μM) evoked relaxation during KPSS-evoked contraction in wild type (WT, black) and TRPM8 knockout mice (TRPM8 KO, purple). (E) Cumulative dataset measuring (S)-PZQ (50μM) evoked relaxation from experiments such as shown in (D). Data represent mean±s.e.m. from averaged measurements from mesenteric vessel strips from n≥3 mice.