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首页> 外文期刊>Psychoneuroendocrinology: An International Journal >An angiotensin-1 converting enzyme polymorphism is associated with allostatic load mediated by C-reactive protein, interleukin-6 and cortisol.
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An angiotensin-1 converting enzyme polymorphism is associated with allostatic load mediated by C-reactive protein, interleukin-6 and cortisol.

机译:血管紧张素1转换酶的多态性与C反应蛋白,白介素6和皮质醇介导的异源负荷有关。

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Allostatic load (AL) is a theoretical framework that describes the cumulative physiologic effects of adaptation to change or stress throughout the lifespan. AL is operationalized by a composite index of multiple biomarkers. Accordingly, genes, behavior and environment contribute to AL. To determine if individual differences in AL may be influenced by inherent genetic variation, we calculated an allostatic load index (ALI) for 182 Caucasian subjects derived from a population-based study of chronic fatigue syndrome. Nearly 65% of the subjects in this study sample reported fatiguing illness. ALI was calculated based on 11 measures representing metabolic, cardiovascular, inflammatory, hypothalamic-pituitary-adrenal (HPA) axis and sympathetic nervous system (SNS) activities. Subjects were dichotomized into high (ALI > or = 3) or low (ALI < 3) AL groups, and the association between high AL and 129 polymorphisms in 32 genes related to the HPA axis, neurotransmission, inflammation, cardiovascular and metabolic functions were evaluated. Polymorphisms in angiotensin-1 converting enzyme (ACE), corticotropin-releasing hormone receptor 1 (CRHR1), and serotonin receptors (HTR3A and HTR4) were associated with AL (p=0.0007-0.0486), but only one polymorphism, rs4968591, in ACE remained significant after correction for multiple comparisons. The T allele of ACE rs4968591 was more common in subjects with high AL (67.5%) than in subjects with low AL (49.3%) (p=0.0007), and this effect appeared independent of age, sex, body mass index and fatigue status. Additionally, high interleukin-6 (IL-6; p(trend)=0.04), and C-reactive protein (CRP; p(trend)=0.01) levels, as well as low urinary cortisol levels in females (p=0.03) were associated with the T allele, which may result in allele-specific binding of the transcription factor, E2F1. Our results suggest a role for ACE in the bidirectional communication between the central nervous and immune systems in response to stress. Further studies will be needed (a) to replicate the association between AL and ACE polymorphisms in population studies designed to differentiate the effects of sex, age and racial/ethnic background, (b) to evaluate the effect of allele-specific binding of E2F1 at rs4968591, and (c) to examine the role of ACE in the co-regulation of CRP, IL-6 and cortisol.
机译:静态负荷(AL)是一个理论框架,描述了在整个生命周期中适应变化或压力的累积生理效应。通过多种生物标志物的综合索引来实施AL。因此,基因,行为和环境有助于AL。为了确定AL的个体差异是否可能受到固有遗传变异的影响,我们计算了基于人群的慢性疲劳综合症研究得出的182名白人受试者的同种异体负荷指数(ALI)。在本研究样本中,近65%的受试者报告有致病性。 ALI是根据代表代谢,心血管,炎症,下丘脑-垂体-肾上腺(HPA)轴和交感神经系统(SNS)活动的11种指标计算得出的。将受试者分为高(ALI>或= 3)或低(ALI <3)AL组,并评估高AL与32种与HPA轴,神经传递,炎症,心血管和代谢功能有关的基因中的129多态性之间的关联。血管紧张素1转换酶(ACE),促肾上腺皮质激素释放激素受体1(CRHR1)和血清素受体(HTR3A和HTR4)的多态性与AL相关(p = 0.0007-0.0486),但ACE中只有一种多态性rs4968591在进行多次比较校正后,仍然保持显着水平。 ACE rs4968591的T等位基因在高AL(67.5%)患者中比在低AL(49.3%)患者中更为常见(p = 0.0007),并且这种效应与年龄,性别,体重指数和疲劳状态无关。此外,白细胞介素6(IL-6; p(趋势)= 0.04)和C反应蛋白(CRP; p(趋势)= 0.01)高水平以及女性的尿皮质醇水平低(p = 0.03)它们与T等位基因相关,这可能导致转录因子E2F1的等位基因特异性结合。我们的结果表明,ACE在应激反应中在中枢神经系统和免疫系统之间的双向通讯中发挥作用。需要进行进一步的研究(a)在旨在区分性别,年龄和种族/种族背景的人群研究中复制AL和ACE多态性之间的关联,(b)评估E2F1等位基因特异性结合的影响rs4968591,以及(c)检查ACE在CRP,IL-6和皮质醇共调节中的作用。

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