IBS stress reactivity phenotype is associated with blood transcriptome profiles and microstructural and functional brain changes

Jennifer Labus, Desiree Delgadillo, Steve Cole, Chencai Wang, Bruce Naliboff, Lin Chang, Benjamin Ellingson, Emeran Mayer
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Abstract

Background & Aims: Clinical evidence suggests significant interindividual differences in stress reactivity (SR), but biological mechanisms and therapeutic implications of these differences are poorly understood. We aimed to identify the biological basis of increased SR by investigating associations between a psychometric-based phenotype with blood transcriptomics profiles of increased sympathetic nervous system (SNS) activation and brain imaging phenotypes in irritable bowel syndrome (IBS) participants and healthy controls (HCs). Methods: A cross-sectional observational study design, transcriptomics profiling, multimodal brain imaging, and psychosocial assessments were obtained in 291 female and male IBS participants and HCs. Prior to analyses, unsupervised clustering was applied to derive high and low SR subgroups across participants based on two measures of SR. General linear models tested for SR group differences in clinical and biological parameters. Exploratory analyses examined associations between SR group-specific brain alterations and gene expression. Results: The high, compared to low SR group showed greater cyclic AMP response element-binding protein (CREB) gene expression consistent with tonic SNS activity and proinflammatory changes in whole blood. Brain imaging showed neuroplastic changes in the high SR group consistent with an upregulation of ascending arousal systems and sensory processing and integration regions, and functional connectivity changes in the central autonomic network. SR moderated the sex difference in extraintestinal symptoms. Conclusions: The findings support a model of tonically increased SNS activity as a plausible risk factor for increased autonomic reactivity to psychosocial stressors and low grade immune activation in both IBS and HCs, with a greater prevalence in IBS. These findings may have important implications for personalized treatment interventions in IBS.
肠易激综合征应激反应表型与血液转录组图谱以及大脑微结构和功能变化有关
我们的目的是通过研究肠易激综合征(IBS)患者和健康对照组(HCs)中基于心理测量的表型与交感神经系统(SNS)激活增加的血液转录组学图谱和脑成像表型之间的关联,确定SR增加的生物学基础。研究方法采用横断面观察研究设计,对291名女性和男性肠易激综合征参与者和健康对照者进行了转录组学分析、多模态脑成像和社会心理评估。在进行分析之前,根据两种SR测量方法,对参与者进行了无监督聚类,以得出高SR亚组和低SR亚组。通用线性模型检验了临床和生物参数中的SR组差异。探索性分析检验了SR组特异性大脑改变与基因表达之间的关联。结果显示与低 SR 组相比,高 SR 组的环磷酸腺苷反应元件结合蛋白(CREB)基因表达量更高,这与强直性 SNS 活动和全血中的促炎性变化一致。脑成像显示,高SR组的神经可塑性变化与上升唤醒系统、感觉处理和整合区域的上调以及中枢自律神经网络的功能连接变化一致。SR调节了肠外症状的性别差异。结论这些研究结果支持了SNS活动增强的模型,它是导致肠易激综合征和高血压患者对社会心理压力和低水平免疫激活的自律神经反应性增强的一个合理的风险因素,在肠易激综合征中的发病率更高。这些发现可能会对肠易激综合征的个性化治疗干预产生重要影响。
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