Role of Inflammation in Depressive and Anxiety Disorders, Affect, and Cognition: Genetic and Non-Genetic Findings in the Lifelines Cohort Study.

  1. Naoise Mac Giollabhui
  2. Chloe Slaney
  3. Gibran Hemani
  4. Eimear Foley
  5. Peter van der Most
  6. Ilja Nolte
  7. Harold Snieder
  8. George Davey Smith
  9. Golam Khandaker
  10. Catharina Hartman
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Abstract

Inflammation is associated with a range of neuropsychiatric symptoms; however, the nature of the causal relationship is unclear. We used complementary non-genetic, genetic risk score (GRS), and Mendelian randomization (MR) analyses to examine whether inflammatory markers are associated with affect, depressive and anxiety disorders, and cognition. We tested in ≈ 55,098 (59% female) individuals from the Dutch Lifelines cohort the concurrent/prospective associations of C-reactive protein (CRP) with: depressive and anxiety disorders; positive/negative affect; and attention, psychomotor speed, episodic memory, and executive functioning. Additionally, we examined the association between inflammatory GRSs (CRP, interleukin-6 [IL-6], IL-6 receptor [IL-6R and soluble IL-6R (sIL-6R)], glycoprotein acetyls [GlycA]) on these same outcomes (N max =57,946), followed by MR analysis examining evidence of causality of CRP on outcomes (N max =23,268). In non-genetic analyses, higher CRP was associated with a depressive disorder, lower positive/higher negative affect, and worse executive function, attention, and psychomotor speed after adjusting for potential confounders. In genetic analyses, CRP GRS was associated with any anxiety disorder (β = 0.002, p  = 0.037) whereas GlycA GRS was associated with major depressive disorder (β = 0.001, p  = 0.036). Both CRP GRS (β = 0.006, p  = 0.035) and GlycA GRS (β = 0.006, p  = 0.049) were associated with greater negative affect. Inflammatory GRSs were not associated with cognition, except sIL-6R GRS which was associated with poorer memory (β=-0.009, p  = 0.018). There was weak evidence for a CRP-anxiety association using MR (β = 0.12; p  = 0.054). Genetic and non-genetic analyses provide consistent evidence for an association between CRP and negative affect. These results suggest that dysregulated immune physiology may impact a broad range of trans-diagnostic affective symptoms.

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  1. Version published to 10.21203/rs.3.rs-4379779/v1 on Research Square