Abstract

The volume of subcortical structures represents a reliable, quantitative, and objective phenotype that captures genetic effects, environmental effects such as trauma, and disease effects such as posttraumatic stress disorder (PTSD). Trauma and PTSD represent potent exposures that may interact with genetic markers to influence brain structure and function. Genetic variants, associated with subcortical volumes in two large normative discovery samples, were used to compute polygenic scores (PGS) for the volume of seven subcortical structures. These were applied to a target sample enriched for childhood trauma and PTSD. Subcortical volume PGS from the discovery sample were strongly associated in our trauma/PTSD enriched sample (n = 7580) with respective subcortical volumes of the hippocampus (p = 1.10 × 10−20), thalamus (p = 7.46 × 10−10), caudate (p = 1.97 × 10−18), putamen (p = 1.7 × 10−12), and nucleus accumbens (p = 1.99 × 10−7). We found a significant association between the hippocampal volume PGS and hippocampal volume in control subjects from our sample, but was absent in individuals with PTSD (GxE; (beta = −0.10, p = 0.027)). This significant GxE (PGS × PTSD) relationship persisted (p < 1 × 10−19) in four out of five threshold peaks (0.024, 0.133, 0.487, 0.730, and 0.889) used to calculate hippocampal volume PGSs. We detected similar GxE (G × ChildTrauma) relationships in the amygdala for exposure to childhood trauma (rs4702973; p = 2.16 × 10−7) or PTSD (rs10861272; p = 1.78 × 10−6) in the CHST11 gene. The hippocampus and amygdala are pivotal brain structures in mediating PTSD symptomatology. Trauma exposure and PTSD modulate the effect of polygenic markers on hippocampal volume (GxE) and the amygdala volume PGS is associated with PTSD risk, which supports the role of amygdala volume as a risk factor for PTSD.

Highlights

  • The effects of psychological trauma and posttraumatic stress disorder (PTSD) on society and individual functioning are immense as measured by a 150%increase in rates of unemployment, and a 60% increase in marital dysfunction, along with elevated rates of suicide, anxiety, and depression [1]

  • While we may assume that polygenic scores (PGS) derived from a multi-cohort consortium coordinated analysis of subcortical normative sample captures the most relevant genetic markers that regions with a standard processing pipeline in 1868 subjects influence subcortical volume, it is possible that heretofore indicated that evidence was strongest for lower hippocampal unknown genetic markers interact with trauma and illness to volume in PTSD [4, 5]

  • We modeled the association between the hippocampal volume and PGS, which were based on the hippocampal Enhancing NeuroImaging Genetics with Meta-Analysis (ENIGMA)-genome-wide association studies (GWAS)-2015 and the hippocampal ENIGMA-GWAS-2017 [22, 26]

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Summary

Introduction

The effects of psychological trauma and PTSD on society and individual functioning are immense as measured by a 150%increase in rates of unemployment, and a 60% increase in marital dysfunction, along with elevated rates of suicide, anxiety, and depression [1]. PTSD include impaired memory, fragmented autobio- examine the role of genetic and environmental effects such as graphical and trauma-related memories [2]. Psychological trauma and PTSD represent involved in discrete aspects of memory encoding and consolida- potent environmental exposures that may interact with genetic tion. Extinction failure suggest that the hippocampus plays a role in Modulation of the PGS by environmental or disease contributors developing PTSD [3]. While we may assume that PGS derived from a multi-cohort consortium coordinated analysis of subcortical normative sample captures the most relevant genetic markers that regions with a standard processing pipeline in 1868 subjects influence subcortical volume, it is possible that heretofore indicated that evidence was strongest for lower hippocampal unknown genetic markers interact with trauma and illness to volume in PTSD [4, 5]

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