Subjects

Thirty-four euBD were recruited from the psychiatric outpatient department at National Cheng Kung University Hospital, while 55 individuals were recruited from the community to the healthy control (HC) group through advertisements. All participants were between 18 and 65 years of age and were recruited and evaluated by an attending psychiatrist using the Chinese version of the Mini International Neuropsychiatry Interview (Sheehan et al., Reference Sheehan, Lecrubier, Sheehan, Amorim, Janavs, Weiller and Dunbar1998). Symptom severity was evaluated by the 17-item Hamilton Depression Rating Scale (HDRS) and the 11-item Young Mania Rating Scale (YMRS); euthymic state was defined as both YMRS and HDRS equal to or lower than 7.

To determine eligibility, all patients were diagnosed by a psychiatrist according to the Diagnostic and Statistical Manual of Mental Disorders, Five Edition (DSM-V). The exclusion criteria for all participants were as follows: (1) major mental illnesses except BD for the patient group; (2) a history of head trauma, organic mental disease, or other neurological disorders; (3) inflammatory diseases, serious surgical conditions, or severe physical illnesses, such as acute coronary syndrome, kidney dialysis, or transplant; and (4) plans for pregnancy, breastfeeding, or a positive pregnancy test.

The study was conducted in accordance with the Declaration of Helsinki and was approved by the Institutional Review Board of National Cheng Kung University Hospital. All participants provided written informed consent prior to their inclusion in the study. After enrollment in the study, administration of medications, such as valproic acid or lithium mood stabilizers, was tracked.

The sample size was calculated based on an effect size reported from a previous study by Scotti-Muzzi et al. (Reference Scotti-Muzzi, Chile, Moreno, Pastorello, da Costa Leite, Henning and Soeiro-de-Souza2021), the Glx/GABA group difference was reported with a partial eta squared (η ²p) of 0.064 (alpha = 0.05, 1-beta = 0.6, as analyzed using G*Power 3.1), which resulted in the estimated number of 81 subjects in total. Aiming for a comparable effect size, we set a recruitment goal of 41 participants per group.

Image acquisition and processing

All participants were scanned using a 3.0 Tesla MRI scanner (GE Discovery MR750, GE Medical Systems, Milwaukee, WI, USA) with an 8-channel head coil in the Mind Research and Imaging Center of National Cheng Kung University. MRS was performed to assess the excitatory glutamate-glutamine (Glx) concentration. A 3-dimensional T1-weighted inversion recovery magnetic resonance imaging (MRI) scan was performed on all subjects (axial MRI 3D brain volume, echo time [TE] = 2.9 ms, repetition time [TR] = 7.7, inversion time = 450 ms, flip angle = 12°, field of view = 230 mm, matrix size = 256 × 256, and slice thickness = 1.0 mm).

¹H-MRS was acquired using point-resolved spectroscopy (PRESS) (TE = 35 ms, TR = 2000 ms, spectral width = 2500 Hz, 2048 data points, 128 water-suppressed, 16 water-unsuppressed averages, and eight excitation numbers) for Glx analysis. A MeshcherGarwood point-resolved spectroscopy (MEGA-PRESS) pulse sequence (TR = 2000 ms, TE = 68 ms, NEX = 8, NS = 128, no water suppression) was performed for GABA analysis. The voxels were placed in the bilateral PCC/PCu (voxel size = 36 × 24 × 32) and mPFC/ACC (voxel size = 25 × 25 × 30), scanned for 9:20. The coordinates of mPFC/ACC voxels (Kegeles et al., Reference Kegeles, Mao, Stanford, Girgis, Ojeil, Xu and Shungu2012) and PCC/PCu voxels (Hu et al., Reference Hu, Chen, Gu and Yang2013) were used. The detailed voxel placement procedures, locations of ¹H-MRS voxels, and representative spectra are shown in Fig. 1. Water-suppressed spectra of mPFC/ACC and PCC/PCu were analyzed using LCModel version 6.3-1K. In the current work, neurometabolites of interest included Glx (glutamate + glutamine) and GABA. As supplemental neurometabolites, myoinositol, glycerophosphocholine + phosphocholine, N-acetylaspartate + N-acetylaspartylglutamate (NAAx), and creatine + phosphocreatine were also collected. All the LCModel spectrum outputs were visually checked. The current study set Cramér-Rao lower bound (CRLB) threshold as <20% to ensure relatively reliable fitting results for further analysis of metabolites.

Figure 1. Voxel locations and placement procedures for ¹H-MRS. (a) Voxel placement in the medial prefrontal cortex/anterior cingulate cortex (mPFC/ACC). (b) Voxel placement in the posterior cingulate cortex/precuneus (PCC/PCu). (c) and (d) Magnetic resonance spectroscopy (MRS) spectra indicating glutamate/glutamine complex (Glx), gamma-aminobutyric acid (GABA), N-acetyl-aspartate (NAA), and N-acetyl-aspartyl-glutamate (NAAG) peaks. ¹H-MRS, proton magnetic resonance spectroscopy.

A partial volume correction was applied to account for tissue concentration in individual voxels. T1-weighted images were segmented into grey matter, white matter, and cerebrospinal fluid using Gannet (version 3.3.2) (https://github.com/markmikkelsen/Gannet), so tissue content within the MRS voxels could be assessed. This study utilized Gannet to create a mask of the voxel size and location on the segmented T1-weighted image, incorporating the spatial coordinates from the scanner. Correction of neurometabolite levels for fraction of cerebrospinal fluid in the region of interest (ROI) was performed using a MATLAB-based package, MRSParVolCorr toolbox (https://github.com/DrMichaelLindner/MRSParVolCo) (Lindner, Bell, Iqbal, Mullins, & Christakou, Reference Lindner, Bell, Iqbal, Mullins and Christakou2017).

The excitatory neurometabolite was defined as Glx (glutamate + glutamine), and the inhibitory neurometabolite was GABA. In this study, the E/I ratios in mPFC/ACC and PCC/PCu were calculated as Glx/GABA.

Wisconsin card-sorting test (WCST)

The computerized version of the WCST (consisting of 64 cards) was administered by an experienced clinical neuropsychologist to evaluate executive function. Participants were instructed to match response cards to four stimulus cards based on color, form, or number along one of the three dimensions at a time. Feedback was provided as either correct or incorrect. The subjects received no information about the dimensions beforehand. After successfully sorting ten cards in one category the rule automatically changed. Participants had to learn to sort cards according to the new category by feedback. Performance was assessed by examining indexes of completed categories and preservative errors (Stratta et al., Reference Stratta, Daneluzzo, Prosperini, Bustini, Mattei and Rossi1997; Volkow et al., Reference Volkow, Gur, Wang, Fowler, Moberg, Ding and Logan1998).

Continuous performance test (CPT)

The CPT is a psychological test to measure attention (Chen, Hsiao, Hsiao, & Hwu, Reference Chen, Hsiao, Hsiao and Hwu1998; Hsieh et al., Reference Hsieh, Chu, Yang, Yang, Yeh, Lee and Chen2005). The target stimulus may be defined either as one particular stimulus out of the available set (X task: participants were asked to respond to number ‘9’) or a particular sequence of two stimuli out of the available set (AX task: participants were asked to respond whenever the number ‘9’ was preceded by the number ‘1’). Only the AX task was used in the present study. The test session began with a 2-min practice period (repeated if participants required it) to ensure that participants knew how to perform the task correctly. During the test, numbers from 0 to 9 were randomly presented for 50 ms each, at a rate of one per second. A total of 331 trials, 34 (10%) of which were target stimuli, were presented over 5 min. Participant responses were recorded automatically on a diskette using the CPT machine (Sunrise Systems, version 2.20, Pembroke, MA, USA) (Smid, de Witte, Homminga, & van den Bosch, Reference Smid, de Witte, Homminga and van den Bosch2006). The rater monitored the performance of each participant through the computer monitor. The index of detectability (d′), which measures the respondent's ability to differentiate non-targets from targets, was used as a measure of attentional function.

Statistical analyses

The demographic and clinical characteristics of the groups of participants were compared using One-way analysis of co-variance (ANCOVA) and chi-squared test. Considering the group difference in age, sex, and years of education, one-way ANCOVA was used to evaluate group differences in neurometabolite levels in the mPFC/ACC and PCC/PCu, behavioral measures and questionnaires controlling for age, sex, and years of education. Supplementary analysis was used to test the robustness of the main finding in selected participants matched for age and sex. Shapiro–Wilk tests were conducted to examine the data distribution of metabolites. Pearson's correlation was used exploratorily to assess the association between E/I ratios in the mPFC/ACC and PCC/PCu and executive function and attention. Regression analyses were performed to explore the potential contributions of different neurometabolites and E/I ratio to cognitive functions. The threshold for statistical significance in group comparisons was adjusted using the Bonferroni correction for two brain regions (threshold p = 0.05/2 = 0.025). The threshold for exploratory association analyses was set at p < 0.05. All statistical analyses were conducted using IBM SPSS Statistics, version 22 (IBM Corporation, Armonk, NY, USA).