Magnetic resonance imaging acquisition and preprocessing

From the original NSPN cohort, a random subset of participants completed neuroimaging, of whom data were available from 117 who had also undertaken the subsequent round collecting the ICBC data. The study was approved by the Cambridge East Research Ethics Committee (approval number 207190), and individuals provided informed consent.

Brain scans were conducted at three sites: two at the University of Cambridge (the Wolfson Brain Imaging Centre and the Medical Research Council Cognition & Brain Sciences Unit) and one at University College London (the Wellcome Trust Functional Imaging Laboratory). All sites had identical 3 T, 32-channel magnetic resonance imaging (MRI) systems (Magnetom TIM Trio) and a unified acquisition sequence. Resting-state functional scans were obtained with a multi-echo echoplanar imaging sequence. Scanner detail and preprocessing steps can be found in the study published by Váša et al.^{Reference Váša, Romero-Garcia, Kitzbichler, Seidlitz, Whitaker and Vaghi6}

Parcellation and network-based statistics analysis

Following preprocessing, functional MRI images were parcellated by subdividing the Desikan–Killiany anatomical atlas into 308 cortical parcels of approximately equal surface area (around 500 mm²) and 16 subcortical regions. Blood oxygenation level dependent time series were estimated from the average over all voxels within each of the 324 parcels (nodes). Pearson correlation was calculated between the time series of each pair of nodes, to determine their functional connectivity strength, resulting in a symmetric 324 × 324 connectivity matrix for each participant (Fig. 1). The resultant matrices were Fisher's r-to-z transformed to improve normality of the correlation estimates.

Fig. 1 (a) Average functional magnetic resonance imaging (fMRI) connectivity matrix. (b) Subnetwork showing reduced functional connectivity associated with latent disinhibition phenotype, assessed with the network-based statistics (NBS) software package and visualised with BrainNet Viewer. (c) The subnetwork consists of 15 edges across 15 regions, connecting the right pars opercularis (in deep blue) to bilateral lateral occipital regions (in red and light blue), the right lateral occipital region to the right supramarginal region (in pink), and the right pars opercularis to the left precentral (in yellow) and left superior frontal gyri (in green), respectively. lLOC, left lateral occipital; lPrg, left precentral gyrus; lSFg, left superior frontal gyrus; rLOC, right lateral occipital; rPOp, right pars opercularis; rSMg, right supramarginal.

The network-based statistics connectome software package (version 1.2; https://www.nitrc.org/projects/nbs/) was used to assess for association between interregional connectivity matrix and disinhibition scores, controlling for age, gender and IQ. IQ was recorded with the Wechsler Abbreviated Scale of Intelligence – Second Edition (WASI-II)^{Reference Wechsler7}. This first included mass univariate testing at each edge, with a primary component-forming threshold of P < 0.0001 uncorrected. Each identified component (i.e. topologically connected subnetwork) was then assessed at 10 000 permutations, using a family-wise error rate-corrected level of P < 0.05.

Graph theory analysis

Graph theoretic analysis (i.e. modelling the brain network as a graph of interconnected regions/nodes) was further used to examine specific brain connection properties. The Brain Connectivity Toolbox^{Reference Rubinov and Sporns8} was used, and properties examined include local network properties (nodal degree, normalised betweenness centrality, local efficiency and clustering coefficient) and global network properties (global efficiency and transitivity). These properties were examined across sparsity thresholds of 0.05 to 0.2 (at increments of 0.01). The areas under the curve across the threshold range for the listed properties were computed, and partial correlation was used to determine if any of these network properties were significantly associated with disinhibition, again controlling for age, gender and IQ. Local and global properties were assessed at P < 0.000154 and P < 0.025, respectively (i.e. Bonferroni-corrected for number of nodes and number of global properties, respectively).