Structural brain characteristics of current co-occurring chronic pain and depression: a cross-sectional analysis of UK Biobank

Background Chronic pain and depression are prevalent and burdensome conditions that frequently co-occur. Separate neuroimaging studies of each disorder suggest overlapping brain-structure alterations, however, relatively few studies have examined their comorbidity directly, and the neuroanatomical profile of co-occurring chronic pain and depression remains unclear. Methods Using UK Biobank data (n = 71,214), we conducted cross-sectional pairwise association analyses of brain structure (cortical measures, subcortical volumes, and white matter microstructure) comparing participants with current comorbid chronic pain and depression, current chronic pain only, current depression only, and controls. Results Compared with controls, the comorbidity group showed regional differences in cortical surface area and thickness ({beta} range = -0.096 to 0.098, pFDR < 0.05), widespread lower cortical volume ({beta} range = -0.096 to -0.050, pFDR < 0.05), lower thalamic (left: {beta} = -0.048, pFDR = 0.038; right: {beta} = -0.060, pFDR = 0.007), hippocampal (left: {beta} = -0.062, pFDR = 0.035; right: {beta} = -0.088, pFDR = 0.002) and left accumbens volume ({beta} = -0.073, pFDR = 0.011), and evidence of widespread white matter microstructure alterations (fractional anisotropy: {beta} range = -0.116 to -0.080, pFDR < 0.05; mean diffusivity: {beta} range = 0.063 to 0.137, pFDR < 0.05). Pairwise comparisons with the disorder-specific groups also identified several alterations unique to the comorbidity group. Compared to controls, those with chronic pain only had widespread lower cortical surface area and volume ({beta} range = -0.043 to -0.015, pFDR < 0.05), whereas non-comorbid depression showed more regionally specific lower cortical thickness and volume ({beta} range = -0.140 to -0.062, pFDR < 0.05) and lower thalamic volume (left: {beta} = -0.067, pFDR = 0.016; right: {beta} = -0.066, pFDR = 0.015), alongside widespread white matter microstructure deficits (fractional anisotropy: {beta} range = -0.104 to -0.083, pFDR < 0.05; mean diffusivity: {beta} range = 0.079 to 0.149, pFDR < 0.05). Conclusion These results provide a robust characterisation of brain structure alterations in comorbid chronic pain and depression, highlighting a distinct neuroanatomical profile and advancing understanding of its underlying neurobiology.