针对性排斥反应会根据社会地位引发青少年体内促炎和抗炎基因表达的差异。
Targeted Rejection Triggers Differential Pro- and Anti-Inflammatory Gene Expression in Adolescents as a Function of Social Status.
作者信息
Murphy Michael L M, Slavich George M, Rohleder Nicolas, Miller Gregory E
机构信息
Department of Psychology, University of British Columbia.
出版信息
Clin Psychol Sci. 2013 Jan;1(1):30-40. doi: 10.1177/2167702612455743.
Abstract
Social difficulties during adolescence influence life-span health. To elucidate underlying mechanisms, we examined whether a noxious social event, targeted rejection (TR), influences the signaling pathways that regulate inflammation, which is implicated in a number of health problems. For this study, 147 adolescent women at risk for developing a first episode of major depression were interviewed every 6 months for 2.5 years to assess recent TR exposure, and blood was drawn to quantify leukocyte messenger RNA (mRNA) for nuclear factor-κB (NF-κB) and inhibitor of κB (I-κB) and the inflammatory biomarkers C-reactive protein and interleukin-6. Participants had more NF-κB and I-κB mRNA at visits when TR had occurred. These shifts in inflammatory signaling were most pronounced for adolescents high in perceived social status. These findings demonstrate that social rejection upregulates inflammatory gene expression in youth at risk for depression, particularly for those high in status. If sustained, this heightened inflammatory signaling could have implications for life-span health.
摘要
青春期的社交困难会影响寿命健康。为了阐明潜在机制,我们研究了一种有害的社会事件——针对性排斥(TR)是否会影响调节炎症的信号通路,炎症与许多健康问题有关。在本研究中,对147名有首次发生重度抑郁症风险的青春期女性,每6个月进行一次为期2.5年的访谈,以评估近期的TR暴露情况,并采集血液以量化核因子κB(NF-κB)和κB抑制因子(I-κB)的白细胞信使核糖核酸(mRNA)以及炎症生物标志物C反应蛋白和白细胞介素-6。当发生TR时,参与者在访视时的NF-κB和I-κB mRNA更多。对于感知社会地位较高的青少年,炎症信号的这些变化最为明显。这些发现表明,社会排斥会上调有抑郁症风险的年轻人的炎症基因表达,尤其是那些地位较高的人。如果这种情况持续下去,这种增强的炎症信号可能会对寿命健康产生影响。
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