Childhood adversity is associated with longitudinal white matter changes after adulthood trauma.

IF 4.8
Tianyi Li, Megan E Huibregtse, Timothy D Ely, Sanne J H van Rooij, Lauren A M Lebois, E Kate Webb, Tanja Jovanovic, Stacey L House, Steven E Bruce, Francesca L Beaudoin, Xinming An, Thomas C Neylan, Gari D Clifford, Sarah D Linnstaedt, Kenneth A Bollen, Scott L Rauch, John P Haran, Alan B Storrow, Christopher Lewandowski, Paul I Musey, Phyllis L Hendry, Sophia Sheikh, Christopher W Jones, Brittany E Punches, Lauren A Hudak, Jose L Pascual, Mark J Seamon, Elizabeth M Datner, Claire Pearson, David A Peak, Roland C Merchant, Robert M Domeier, Niels K Rathlev, Brian J O'Neil, Paulina Sergot, Leon D Sanchez, John F Sheridan, Ronald C Kessler, Karestan C Koenen, Kerry J Ressler, Samuel A McLean, Jennifer S Stevens, Nathaniel G Harnett
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Abstract

Background: Childhood adversity is associated with susceptibility to posttraumatic stress disorder (PTSD) in adulthood. PTSD and childhood adversity are linked to white matter microstructure, yet the role of white matter as a potential neural mechanism connecting childhood adversity to PTSD remains unclear. The present study investigated the potential moderating role of previous childhood adversity on longitudinal changes in white matter microstructure and posttraumatic stress symptoms following a recent traumatic event in adulthood.

Methods: As part of the AURORA Study, 114 recent trauma survivors completed diffusion weighted imaging at 2-weeks and 6-months after exposure. Participants reported on prior childhood adversity and PTSD symptoms at 2-weeks, 6-months, and 12-months post-trauma. We performed both region-of-interest (ROI) using fractional anisotropy (FA) and whole-brain correlational tractography using quantitative anisotropy (QA) analyses to index associations between white matter microstructure changes and prior adversity.

Results: ROI-based analyses did not identify significant associations between childhood adversity and changes in FA. Whole-brain correlational tractography revealed that greater childhood adversity moderated the QA changes within threat and visual processing tracts including the cingulum bundle and inferior fronto-occipital fasciculus (IFOF). QA changes within cingulum bundle and IFOF were associated with changes in PTSD symptoms between 2-weeks and 6-months.

Conclusions: Our findings suggest temporal variability in threat and visual white matter tracts may be a potential neural pathway through which childhood adversity confers risk to PTSD symptoms after adulthood trauma. Future studies should take the temporal properties of white matter into consideration to better understand the neurobiology of childhood adversity and PTSD.

童年逆境与成年创伤后的纵向白质变化有关。
背景:童年逆境与成年后创伤后应激障碍(PTSD)的易感性相关。创伤后应激障碍和童年逆境与白质微观结构有关,但白质作为连接童年逆境与创伤后应激障碍的潜在神经机制的作用尚不清楚。本研究探讨了童年逆境对成年后近期创伤事件后白质微观结构纵向变化和创伤后应激症状的潜在调节作用。方法:作为AURORA研究的一部分,114名近期创伤幸存者在暴露后2周和6个月完成弥散加权成像。参与者在创伤后2周、6个月和12个月报告了之前的童年逆境和PTSD症状。我们使用分数各向异性(FA)进行感兴趣区域(ROI)分析,并使用定量各向异性(QA)分析全脑相关神经束成像,以确定白质微结构变化与先前逆境之间的关联。结果:基于roi的分析没有发现童年逆境和FA变化之间的显著关联。全脑相关神经束造影显示,童年时期更大的逆境调节了包括扣带束和额枕下束在内的威胁束和视觉加工束(IFOF)内的QA变化。2周至6个月间,扣带束内QA变化和IFOF与PTSD症状变化相关。结论:我们的研究结果表明,威胁和视觉白质束的时间变异可能是童年逆境对成年创伤后PTSD症状风险的潜在神经通路。未来的研究应考虑到白质的时间特性,以更好地了解童年逆境和创伤后应激障碍的神经生物学。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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