UDTR employs different rules that converge on specific levels of accuracy. We used a three-up, one-down rule, meaning that for three consecutive hits we adjusted the stimulus one step harder and for any miss we adjusted the stimulus one step easier. This rule necessarily selleck kinase inhibitor converges on an accuracy level of 79.4%. During the experimental session, participants were instructed to respond as quickly and accurately
as possible to the detection of targets within the cued modality and to withhold responses otherwise. Participants were further instructed to refrain from eyeblinks during each trial as much as possible. Each participant completed one visual and one auditory pure-task block of 100 trials, followed by ~20 mixed-task blocks of 30 trials AZD6738 each, resulting in the collection of ~300 trials per cue condition. Continuous EEG was recorded, with a bandpass of DC to 134 Hz, from 168 scalp electrodes (Biosemi ActiveTwo System, Amsterdam, Netherlands) at an analog-to-digital sampling rate of 512 Hz. Biosemi replaces the ground electrodes that are used in conventional systems with two separate electrodes: a Common Mode Sense and a Driven Right Leg passive electrode. These two electrodes
create a feedback loop, thus rendering them references. With the Biosemi system, every electrode or combination of electrodes can be assigned as a reference, which is done purely in software after acquisition. EEG data were processed using
the FieldTrip toolbox Vitamin B12 (Donders Institute for Brain, Cognition and Behaviour, Radboud University Nijmegen, The Netherlands). This MATLAB (The MathWorks Inc., Natick, MA, USA) toolbox and supporting materials can be accessed at http://www.ru.nl/neuroimaging/fieldtrip. The continuous EEG data were stored and then re-referenced to the average reference and low-pass filtered with a cutoff frequency of 40 Hz. Trials with blinks and excessive eye movements were rejected based on the horizontal and vertical electro-occulogram. Over all other electrodes, a trial rejection threshold of ±100 μV was used. Trials were then epoched from −200 to +1805 ms around the onset of the S1 cue-stimulus. The period of −100 to 0 ms was defined as baseline. To obtain so-called global switching costs, we quantified the difference in reaction times (RTs) and response accuracy (d-prime; see below) between mixed and pure task blocks. To obtain local switching costs, we analysed differences in RT and d-prime between switch and repeat trials within the mixed blocks. The RT was measured from all correct ‘go’ trials (i.e. trials with a target in the cued modality). Responses were only considered valid if they occurred in the window 200–1500 ms following the onset of the gabor in attend-visual conditions and the second tone stimulus in the attend-auditory conditions.