Kinetic modelling of testosterone-related differences in the hypothalamic–pituitary–adrenal axis response to stress

IF 1.7 4区 化学 Q4 CHEMISTRY, PHYSICAL Reaction Kinetics, Mechanisms and Catalysis Pub Date : 2017-11-17 DOI:10.1007/s11144-017-1315-7
Ana Stanojević, Vladimir M. Marković, Stevan Maćešić, Ljiljana Kolar-Anić, Vladana Vukojević
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引用次数: 12

Abstract

The sex hormone testosterone (TTS) and the hypothalamic–pituitary–adrenal (HPA) axis mutually control one another’s activity, wherein TTS suppresses corticotrophin releasing hormone (CRH) stimulated HPA axis activity, whereas?the activation of HPA axis has an inhibitory effect on TTS secretion. With an intention to explain these phenomena, a network reaction model is developed from the previously postulated stoichiometric models for HPA activity where main dynamic behaviors are controlled by two catalytic steps (one autocatalytic and one autoinhibitory) with respect to cortisol, both found experimentally. The capacity of the model to emulate TTS effects on HPA axis dynamics and its response to acute CRH-induced stress is examined using numerical simulations. Model predictions are compared with empirically obtained results reported in the literature. Thus, the reaction kinetic examinations of nonlinear biochemical transformations that constitute the HPA axis, including the negative feedback effect of TTS on HPA axis activity, recapitulates the well-established fact that TTS dampens HPA axis basal activity, decreasing both cortisol level and the amplitude of ultradian cortisol oscillations. The model also replicates TTS inhibitory action on the HPA axis response to acute environmental challenges, particularly CRH-induced stress. In addition, kinetic modelling revealed that TTS induced reduction in ultradian cortisol amplitude arises because the system moves towards a supercritical Hopf bifurcation as TTS is being increased.

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下丘脑-垂体-肾上腺轴对应激反应中睾酮相关差异的动力学模型
性激素睾酮(TTS)和下丘脑-垂体-肾上腺(HPA)轴相互控制彼此的活动,其中TTS抑制促肾上腺皮质激素释放激素(CRH)刺激HPA轴的活动,而?HPA轴的激活对TTS的分泌有抑制作用。为了解释这些现象,我们从先前假设的HPA活性的化学计量模型中开发了一个网络反应模型,其中主要的动力学行为是由两个催化步骤(一个自催化和一个自抑制)控制的,这两个步骤都是通过实验发现的。模型模拟TTS对HPA轴动力学的影响及其对急性crh诱导应力的响应的能力通过数值模拟进行了检验。将模型预测结果与文献中报道的经验结果进行比较。因此,对构成HPA轴的非线性生化转化的反应动力学检查,包括TTS对HPA轴活性的负反馈效应,概括了一个公认的事实,即TTS抑制HPA轴的基础活性,降低皮质醇水平和超周皮质醇振荡的幅度。该模型还复制了TTS对HPA轴对急性环境挑战的抑制作用,特别是crh诱导的应激。此外,动力学模型显示,随着TTS的增加,系统向超临界Hopf分岔移动,TTS诱导的超肽皮质醇振幅降低。
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来源期刊
CiteScore
3.30
自引率
5.60%
发文量
201
审稿时长
2.8 months
期刊介绍: Reaction Kinetics, Mechanisms and Catalysis is a medium for original contributions in the following fields: -kinetics of homogeneous reactions in gas, liquid and solid phase; -Homogeneous catalysis; -Heterogeneous catalysis; -Adsorption in heterogeneous catalysis; -Transport processes related to reaction kinetics and catalysis; -Preparation and study of catalysts; -Reactors and apparatus. Reaction Kinetics, Mechanisms and Catalysis was formerly published under the title Reaction Kinetics and Catalysis Letters.
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