Nagatomo K , Kubo Y .

             response to caffeine

Fig.2. Caffeine-induced currents in Xenopus oocytes expressing mTRPA1. (A) Current recordings were obtained under 2-electrode voltage clamp by applying step pulses to +60 mV from a holding potential of −20 mV repeatedly every 2 s, before and after application of agonists. Responses to 5 mM caffeine (Top), 100 μM AITC (Middle), and 400 μM menthol (Bottom) are shown. (B) Time course of the change in peak current amplitude after application of agonists. (C and D) Current–voltage relationship for responses to the indicated concentrations of caffeine. (C) During the steady state after 30-s exposure to the indicated concentrations of caffeine, 300-ms step pulses from −80 to +80 mV were applied and then stepped back to +60 mV for 100 ms every 1 s from the holding potential of −20 mV. (D) y axis shows the current amplitudes at the indicated membrane potentials in the presence of caffeine (0.1–10 mM). (Inset) An expanded view of the voltage range at which inward current was observed. The n values indicate numbers of recorded oocytes, and the plots depict mean ± SEM.

Fig.6. Current recordings from Xenopus oocytes expressing hTRPA1. Using a 2-electrode voltage clamp, 200-ms ramp pulses from −100 to +100 mV were applied every 5 s from a holding potential of −60 mV to oocytes expressing mTRPA1 (A and C) or hTRPA1 (B and D). Agonists were applied at the times indicated by the bars. (A and C) Responses of mTRPA1 to both caffeine and AITC were confirmed; C is an expanded view of the boxed region in A. (B and D) The response of hTRPA1 to AITC was confirmed, but a decrease in the current amplitude was observed upon application of caffeine. The suppression was more clearly observed when basal channel current was increased by application and washout of AITC (B; expanded in D) or in the presence of AITC (B). Recordings similar to A and B were obtained from 3 cells, and representative data are shown.

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