Study population

This is a post hoc exploratory analysis of prospectively collected trial data from 33 depressed patients treated with ECT in Rijnstate Hospital (Arnhem, The Netherlands), who participated in the StudY of effect of Nimodipine and Acetaminophen on Postictal Symptoms after ECT (SYNAPSE; NCT04028596). SYNAPSE was a randomized controlled trial with a three-condition crossover design. Patients received nimodipine, acetaminophen, or placebo (i.e., water) in a random and counterbalanced order at a maximum of 2 hours before each ECT session [Reference Verdijk, Pottkämper, Verwijk, van Wingen, van Putten and Hofmeijer19]. Repeated EEG measures before, during, and until 1 hour after the ECT sessions were collected to study the effects of the various treatment conditions on postictal recovery. Inclusion criteria for patients were age ≥18 years and having a current clinical diagnosis of major depression (i.e., classified as unipolar, bipolar, and schizoaffective disorder, according to the Diagnostic Manual of Mental Disorders, fifth edition [DSM-5]) [20]. The local medical ethical committee approved the study protocol (NCT04028596), and all included patients provided oral and written informed consent.

ECT and treatment outcome measures

ECT was administered according to the Dutch treatment guidelines in the context of current care, twice a week, and electrodes were either placed right unilateral (RUL) or bi(fronto)temporal (BL) [Reference van den Broek, Birkenhäger, de Boer, Burggraaf, van Gemert and Groenland21]. ECT stimuli were delivered with a constant current (900 mA), square wave, bidirectional, and brief pulse (1 millisecond) using the Thymatron System IV device (Somatics Incorporation, Lake Bluff, Illinois, USA). In case patients showed a poor response initially, RUL placement was switched to BL placement. Anesthesia was mostly achieved using etomidate (0.2–0.3 mg/kg body weight) for sedation and succinylcholine (0.5–1 mg/kg) for muscle relaxation. In case of severe postictal confusion, defined as the clinical necessity to administer sedatives or restraints due to severe motor restlessness, disorientation, agitation, or anxiety [Reference Schuur, PAJ Verdijk, ten Doesschate, van Wingen and van Waarde22]), midazolam (2.5–5 mg intravenously) was used. Cessation of the ECT course was clinically decided by the treating psychiatrists and rated with the Hamilton Depression Rating Scale (HDRS) [Reference Hamilton23]. Clinical response was defined as a decrease of ≥50% of post-ECT HDRS score compared to pre-ECT, and remission was defined as a post-ECT HDRS score <8.

EEG registration and preprocessing

Twelve or 20 silver/silver chloride cup electrodes were placed on the scalp according to the International 10–20 system. Cz was used as a reference. The electrode-skin impedance was kept below 5 kΩ. EEG was recorded before, during, and after the seizure: recordings started around 5 minutes before the administration of anesthesia and lasted up to 1 hour after seizure termination. In this study, both ictal and postictal EEG recordings were used. Data were band-pass filtered (0.5–30 Hz; first-order Butterworth filter) and segmented into 5-second epochs without artifacts. EEG recordings were visually inspected for artifacts by NeuroCenter EEG software (Leiden, The Netherlands). Electrodes containing noise or electrodes that were physically removed during the measurements (e.g., due to movement or postictal agitation) were rejected for analyses. All EEG analyses, preprocessing steps, and fits were conducted with MATLAB R2023a (MathWorks, Natick, MA, USA).

Restoration of the postictal EEG

The start of the postictal state was defined at seizure termination, which was based on the cessation of spike-wave complexes and EEG suppression. Restoration of the postictal EEG was quantified with the normalized alpha–delta ratio (ADR), which was calculated and expressed as follows:

(1) $$ ADR=\frac{pow\left(\alpha \right)- pow\left(\delta \right)}{pow\left(\alpha \right)+ pow\left(\delta \right)}, $$

with $ pow\left(\alpha \right) $ and $ pow\left(\delta \right) $ the power in the alpha (8–13 Hz) and delta (0.5–4 Hz) frequency bands, respectively. These values were calculated from computing power spectral density (PSD) values using Welch’s method [Reference Welch24]. Five-second artifact-free segments with an overlap of 50% were used, and median PSD values were determined for the available electrode channels (whole brain). ADR values were averaged per minute and fitted with a sigmoidal function given by

(2) $$ f(t)=\frac{a}{1+ b{e}^{-\left( c- t\right)/\tau}}+ d, $$

with $ t $ the duration of the postictal state (with a minimum duration of 40 min), $ a $ the distance from $ d $ to the lower asymptote, $ b $ the transition from rapid to reduced growth, $ c $ the initial lag, $ \tau $ the time constant, and $ d $ the upper asymptote. The values of the parameters ( $ a, b, c,\tau $ , and $ d $ ) were estimated using a nonlinear least-squares routine. R² ≥ 0.7 was considered appropriate for goodness of the fit. Subsequently, the derivative (df/dt) of equation 2 was calculated, given by

(3) $$ \frac{df}{dt}=-\frac{ab{ e}^{-\left( c- t\right)/\tau}}{\tau {\left(1+{e}^{-\left( c- t\right)/\tau}\right)}^2} $$

to estimate the timepoint where the recovery of ADR was at its maximum (T_max). T_max was defined as the timepoint where equation 3 had its maximum value. The EEG features we used for postictal EEG restoration were the parameters $ a $ and $ \tau $ from equation 2 and T_max from equation 3.

Seizure duration

Seizure duration was defined as the time interval between seizure onset and offset points, which were determined visually in the EEG. Seizure onset was defined as the onset of rhythmicity of spike-wave complexes, including waveform repetition with relatively uniform morphology and duration. Seizure offset was the timepoint where the seizure terminated, which was defined as the onset of generalized postictal suppression of at least 2 seconds [Reference JCM, PAJ, Stuiver, Aalbregt, Schmettow and Hofmeijer17, Reference Kane, Acharya, Benickzy, Caboclo, Finnigan and Kaplan25, Reference Pottkämper, Verdijk, Hofmeijer, van Waarde and van Putten26].

Recovery of clinical orientation

Before each ECT session, ROT questions were asked to assess orientation at baseline. After the ECT stimulus, ROT questions were asked every 5 minutes to assess recovery of clinical orientation [Reference Sobin, Sackeim, Prudic, Devanand, Moody and McElhiney7]. The ROT questionnaire consists of five questions to assess orientation in person (name, birthday), place (name of hospital), and time (age, day of week). Time to reorientation in all three domains was determined separately by registration of the time (in minutes) until the question regarding a specific cognitive domain was answered correctly for the first time. Since the domains person and time consisted of two questions, these values were averaged, resulting in a single time to reorientation value for each domain. In case patients were not orientated at baseline in a specific domain, this domain was ignored for analysis.

Statistical analyses

Variables were described by using numbers and percentages (%), means and standard deviation, and medians and interquartile range (IQR), as appropriate. Pre- and post-ECT HDRS scores were compared using Wilcoxon’s signed-rank test, with p < 0.05 regarded as statistically significant. Statistical analyses were computed using MATLAB and R version 4.3.1 using the lme4 and report packages [Reference Bates, Mächler, Bolker and Walker27, Reference Makowski, Lüdecke, Patil, Thériault, Ben-Shachar and Wiernik28].