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A Role for Homeostatic Drive in the Perpetuation of Complex Chronic Illness: Gulf War Illness and Chronic Fatigue Syndrome

机译:稳态驱动在复杂慢性疾病永存中的作用:海湾战争疾病和慢性疲劳综合症

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摘要

A key component in the body\u27s stress response, the hypothalamic-pituitary-adrenal (HPA) axis orchestrates changes across a broad range of major biological systems. Its dysfunction has been associated with numerous chronic diseases including Gulf War Illness (GWI) and chronic fatigue syndrome (CFS). Though tightly coupled with other components of endocrine and immune function, few models of HPA function account for these interactions. Here we extend conventional models of HPA function by including feed-forward and feedback interaction with sex hormone regulation and immune response. We use this multi-axis model to explore the role of homeostatic regulation in perpetuating chronic conditions, specifically GWI and CFS. An important obstacle in building these models across regulatory systems remains the scarcity of detailed human in vivo kinetic data as its collection can present significant health risks to subjects. We circumvented this using a discrete logic representation based solely on literature of physiological and biochemical connectivity to provide a qualitative description of system behavior. This connectivity model linked molecular variables across the HPA axis, hypothalamic-pituitary-gonadal (HPG) axis in men and women, as well as a simple immune network. Inclusion of these interactions produced multiple alternate homeostatic states and sexually dimorphic responses. Experimental data for endocrine-immune markers measured in male GWI subjects showed the greatest alignment with predictions of a naturally occurring alternate steady state presenting with hypercortisolism, low testosterone and a shift towards a Th1 immune response. In female CFS subjects, expression of these markers aligned with an alternate homeostatic state displaying hypocortisolism, high estradiol, and a shift towards an anti-inflammatory Th2 activation. These results support a role for homeostatic drive in perpetuating dysfunctional cortisol levels through persistent interaction with the immune system and HPG axis. Though coarse, these models may nonetheless support the design of robust treatments that might exploit these regulatory regimes.
机译:下丘脑-垂体-肾上腺(HPA)轴是机体应激反应的关键组成部分,可协调各种主要生物系统的变化。其功能障碍与许多慢性疾病有关,包括海湾战争病(​​GWI)和慢性疲劳综合症(CFS)。尽管与内分泌和免疫功能的其他成分紧密结合,但很少有HPA功能模型可以解释这些相互作用。在这里,我们通过包括与性激素调节和免疫反应的前馈和反馈相互作用来扩展HPA功能的常规模型。我们使用这种多轴模型来探索稳态调节在长期慢性病(特别是GWI和CFS)中的作用。跨监管系统建立这些模型的一个重要障碍仍然是缺乏详细的人体体内动力学数据,因为其收集可能会给受试者带来重大的健康风险。我们仅基于生理和生化连通性的文献使用离散逻辑表示来规避此问题,以提供系统行为的定性描述。这种连通性模型通过HPA轴,男性的下丘脑-垂体-性腺(HPG)轴以及简单的免疫网络链接分子变量。包括这些相互作用产生了多个交替的稳态和性二态反应。在男性GWI受试者中测得的内分泌免疫标记物的实验数据显示,与自然发生的交替稳定状态的预测具有最大的一致性,该预测状态表现为皮质醇过多,睾丸激素水平低和向Th1免疫应答的转变。在女性CFS受试者中,这些标志物的表达与交替的稳态状态保持一致,显示皮质醇过低,雌二醇含量高,并趋向于消炎性Th2激活。这些结果表明,通过与免疫系统和HPG轴的持续相互作用,稳态驱动在使功能紊乱的皮质醇水平持续存在中发挥了作用。这些模型虽然粗略,但仍可能支持可能利用这些监管制度的稳健治疗方法的设计。

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