创伤周围炎症细胞因子和类固醇激素的性别差异有助于非缓解性创伤后应激障碍的前瞻性风险。

Q1 Psychology Chronic Stress Pub Date : 2021-09-23 eCollection Date: 2021-01-01 DOI:10.1177/24705470211032208

Chloe S Lalonde, Yara Mekawi, Kelly F Ethun, Eleonore Beurel, Felicia Gould, Firdaus S Dhabhar, Katharina Schultebraucks, Isaac Galatzer-Levy, Jessica L Maples-Keller, Barbara O Rothbaum, Kerry J Ressler, Charles B Nemeroff, Jennifer S Stevens, Vasiliki Michopoulos

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引用次数: 9

摘要

与男性相比，女性患创伤后应激障碍(PTSD)的风险更高，但人们对这种性别差异的生物学原因知之甚少。一种可能的机制是对创伤应激暴露的不同免疫和神经内分泌反应。在当前的前瞻性研究中，我们旨在通过促炎标志物确定性别是否与发展为非缓解型PTSD的可能性间接相关，以及类固醇激素浓度是否影响这种效应。从急诊科招募女性(n = 179)和男性(n = 197)创伤幸存者，在创伤暴露后24小时内完成临床评估并在3小时内完成血液样本采集。测定血浆中促炎细胞因子(IL-6、IL-1 β、TNF、IFNγ)和类固醇激素(雌二醇、睾酮、孕酮、皮质醇)浓度。与男性相比，女性在创伤后发生非缓解性PTSD的可能性更高(p = 0.04)，促炎细胞因子和睾酮水平较低(p'sp'sp = 0.24)。促炎细胞因子是性别与发生非缓解型PTSD概率之间关系的重要中介

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Sex Differences in Peritraumatic Inflammatory Cytokines and Steroid Hormones Contribute to Prospective Risk for Nonremitting Posttraumatic Stress Disorder.

Women are at higher risk for developing posttraumatic stress disorder (PTSD) compared to men, yet little is known about the biological contributors to this sex difference. One possible mechanism is differential immunological and neuroendocrine responses to traumatic stress exposure. In the current prospective study, we aimed to identify whether sex is indirectly associated with the probability of developing nonremitting PTSD through pro-inflammatory markers and whether steroid hormone concentrations influence this effect. Female (n = 179) and male (n = 197) trauma survivors were recruited from an emergency department and completed clinical assessment within 24 h and blood samples within ∼three hours of trauma exposure. Pro-inflammatory cytokines (IL-6, IL-1 $β$ , TNF, IFNγ), and steroid hormone (estradiol, testosterone, progesterone, cortisol) concentrations were quantified in plasma. Compared to men, women had a higher probability of developing nonremitting PTSD after trauma (p = 0.04), had lower pro-inflammatory cytokines and testosterone (p's<0.001), and had higher cortisol and progesterone (p's<0.001) concentrations. Estradiol concentrations were not different between the sexes (p = 0.24). Pro-inflammatory cytokines were a significant mediator in the relationship between sex and probability of developing nonremitting PTSD (p < 0.05), such that men had higher concentrations of pro-inflammatory cytokines which were associated with lower risk of nonremitting PTSD development. This effect was significantly moderated by estradiol (p < 0.05), as higher estradiol levels in men were associated with higher pro-inflammatory cytokine concentrations and lower risk for developing nonremitting PTSD. The current results suggest that sex differences in the pro-inflammatory cytokine response to trauma exposure partially mediate the probability of developing nonremitting PTSD, and that the protective ability to mount an pro-inflammatory cytokine response in men may depend on higher estradiol levels in the aftermath of trauma exposure.