Peritraumatic C-reactive protein levels predict pain outcomes following traumatic stress exposure in a sex-dependent manner.

Lauren A McKibben, Miranda N Layne, Liz Marie Albertorio-Sáez, Ying Zhao, Erica M Branham, Stacey L House, Francesca L Beaudoin, Xinming An, Jennifer S Stevens, Thomas C Neylan, Gari D Clifford, Laura T Germine, 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, Robert A Swor, Lauren A Hudak, Jose L Pascual, Mark J Seamon, Elizabeth M Datner, David A Peak, Roland C Merchant, Robert M Domeier, Niels K Rathlev, Brian J O'Neil, Leon D Sanchez, Steven E Bruce, John F Sheridan, Steven E Harte, Ronald C Kessler, Karestan C Koenen, Kerry J Ressler, Samuel A McLean, Sarah D Linnstaedt
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Abstract

Background: Chronic pain following traumatic stress exposure (TSE) is common. Increasing evidence suggests inflammatory/immune mechanisms are induced by TSE, play a key role in the recovery process versus development of post-TSE chronic pain, and are sex specific. In this study, we tested the hypothesis that the inflammatory marker C-reactive protein (CRP) is associated with chronic pain after TSE in a sex-specific manner.

Methods: We utilized blood-plasma samples and pain questionnaire data from men (n=99) and (n=223) women enrolled in AURORA, a multi-site emergency department (ED)-based longitudinal study of TSE survivors. We measured CRP using Ella/ELISA from plasma samples collected in the ED ('peritraumatic CRP', n=322) and six months following TSE (n=322). Repeated measures mixed-effects models were used to assess the relationship between peritraumatic CRP and post-TSE chronic pain.

Results: Peritraumatic CRP levels significantly predicted post-TSE chronic pain, such that higher levels of CRP were associated with lower levels of pain over time following TSE, but only in men (men:β=-0.24, p=0.037; women:β=0.05, p=0.470). By six months, circulating CRP levels had decreased by more than half in men, but maintained similar levels in women (t(290)=1.926, p=0.055). More men with a decrease in CRP levels had decreasing pain over time versus women (men:83% women:65%; Z=2.21, p=0.027).

Conclusions: In men but not women, we found circulating peritraumatic CRP levels predict chronic pain outcomes following TSE and resolution of CRP levels in men over time might be associated with increased pain recovery. Further studies are needed to validate these results.

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背景:创伤应激暴露(TSE)后的慢性疼痛很常见。越来越多的证据表明,TSE 会诱发炎症/免疫机制,这些机制在创伤应激暴露后慢性疼痛的恢复过程和发展过程中起着关键作用,而且具有性别特异性。在本研究中,我们测试了炎症标志物 C 反应蛋白(CRP)与 TSE 后慢性疼痛的相关性与性别特异性的假设:我们利用了参加 AURORA 的男性(人数=99)和女性(人数=223)的血浆样本和疼痛问卷数据,AURORA 是一项基于多站点急诊科(ED)的 TSE 幸存者纵向研究。我们使用 Ella/ELISA 测量了在急诊室采集的血浆样本("创伤周 CRP",人数=322)和 TSE 后 6 个月的 CRP(人数=322)。采用重复测量混合效应模型评估创伤周CRP与TSE后慢性疼痛之间的关系:创伤周CRP水平可显著预测TSE后的慢性疼痛,因此TSE后较高的CRP水平与较低的疼痛水平相关,但仅限于男性(男性:β=-0.24,p=0.037;女性:β=0.05,p=0.470)。六个月后,男性的循环 CRP 水平下降了一半以上,而女性则保持在相似水平(t(290)=1.926,p =0.055)。随着时间的推移,CRP水平下降的男性疼痛减轻的比例高于女性(男性:83%,女性:65%;Z=2.21,P=0.027):结论:我们发现,在男性而非女性中,循环创伤周CRP水平可预测TSE后的慢性疼痛结果,而随着时间的推移,男性CRP水平的降低可能与疼痛恢复程度的增加有关。结论:我们发现男性而非女性的循环创伤周CRP水平可预测TSE后的慢性疼痛结果,而且随着时间的推移,男性CRP水平的下降幅度大于女性。
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