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Modeling the Influence of Chronopharmacological Administration of Synthetic Glucocorticoids on the Hypothalamic-Pituitary-Adrenal Axis

机译:建模慢性糖皮质激素类药物对下丘脑-垂体-肾上腺轴的影响

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摘要

Natural glucocorticoids, a class of cholesterol-derived hormones, modulate an array of metabolic, anti-inflammatory, immunosuppressive and cognitive signaling. The synthesis of natural glucocorticoids, largely cortisol in humans, is regulated by the hypothalamic-pituitary-adrenal (HPA) axis and exhibits pronounced circadian variation. Considering the central regulatory function of endogenous glucocorticoids, maintenance of the circadian activity of the HPA axis is essential to host survival and chronic disruption of such activity leads to systemic complications. There is a great deal of interest in synthetic glucocorticoids due to the immunosuppressive and anti-inflammatory properties and the development of novel dosing regimens that can minimize the disruption of endogenous activity, while still maintaining the pharmacological benefits of long-term synthetic glucocorticoid therapy. Synthetic glucocorticoids are associated with an increased risk of developing the pathological disorders related to chronic suppression of cortisol rhythmicity as a result of the potent negative feedback by synthetic glucocorticoids on the HPA axis precursors. In this study, a mathematical model was developed to explore the influence of chronopharmacological dosing of exogenous glucocorticoids on the endogenous cortisol rhythm considering intra-venous and oral dosing. Chronic daily dosing resulted in modification of the circadian rhythmicity of endogenous cortisol with the amplitude and acrophase of the altered rhythm dependent on the administration time. Simulations revealed that the circadian features of the endogenous cortisol rhythm can be preserved by proper timing of administration. The response following a single dose was not indicative of the response following long-term, repeated chronopharmacological dosing of synthetic glucocorticoids. Furthermore, simulations revealed the inductive influence of long-term treatment was only associated with low to moderate doses, while high doses generally led to suppression of endogenous activity regardless of the chronopharmacological dose. Finally, chronic daily dosing was found to alter the responsiveness of the HPA axis, such that a decrease in the amplitude of the cortisol rhythm resulted in a partial loss in the time-of-day dependent response to CRH stimulation, while an increase in the amplitude was associated with a more pronounced time-of-day dependence of the response.
机译:天然糖皮质激素是一类胆固醇来源的激素,可调节一系列代谢,抗炎,免疫抑制和认知信号。天然糖皮质激素(主要是人类的皮质醇)的合成受下丘脑-垂体-肾上腺(HPA)轴的调控,并表现出明显的昼夜节律变化。考虑到内源性糖皮质激素的中央调节功能,维持HPA轴的昼夜活动对于宿主存活至关重要,并且这种活动的长期破坏会导致全身并发症。由于具有免疫抑制和抗炎特性,并且开发了新的给药方案,可以最大程度地减少内源性活性的破坏,同时仍保持长期合成糖皮质激素治疗的药理学优势,因此合成糖皮质激素引起了人们极大的兴趣。合成糖皮质激素与由于HPA轴前体对合成糖皮质激素的强力负反馈作用而导致与慢性抑制皮质醇节律有关的病理性疾病风险增加有关。在这项研究中,建立了一个数学模型,以探讨考虑静脉内和口服给药时,外源性糖皮质激素的时间药理剂量对内源性皮质醇节律的影响。长期每日给药导致内源性皮质醇的昼夜节律性改变,节律的幅度和顶相取决于给药时间。模拟表明内源性皮质醇节律的昼夜节律特征可以通过适当的给药时间来保留。单剂量后的反应并不表示合成糖皮质激素长期,反复按时间药理学给药后的反应。此外,模拟显示长期治疗的诱导影响仅与低剂量至中剂量有关,而高剂量通常可抑制内源性活性,而与时间药理剂量无关。最后,发现长期每日给药改变了HPA轴的反应性,因此皮质醇节律幅度的减少导致对CRH刺激的时间依赖性反应的部分丧失,而对CRH刺激的依赖性增加。振幅与响应中更明显的时间依赖性相关。

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