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选择吸入性糖皮质激素时的药效学和药代动力学考量

Pharmacodynamic and pharmacokinetic considerations in choosing an inhaled corticosteroid.

作者信息

Colice Gene L

机构信息

Pulmonary, Critical Care and Respiratory Services, Washington Hospital Center, The George Washington University School of Medicine, Washington, DC, USA.

出版信息

Treat Respir Med. 2006;5(4):245-53. doi: 10.2165/00151829-200605040-00003.

Abstract

Inhaled corticosteroids are effective in controlling airway inflammation. Their anti-inflammatory effect is primarily topical, at the site of deposition in the airways. Consequently, traditional pharmacodynamic and pharmacokinetic concepts, which rely on measuring blood concentrations of drug, have limited applicability for evaluating the efficacy of topically acting inhaled corticosteroids. Important factors affecting efficacy of inhaled corticosteroids are: (i) intrinsic properties of the drugs, particularly their affinity for the corticosteroid receptor; and (ii) the newer pharmacodynamic concept of deposition characteristics of the drug formulation. Small particle formulations, especially those developed in the metered-dose inhaler with the new hydrofluoroalkane propellant, deposit to a much greater extent in the lung and may consequently have improved clinical efficacy. Lipid conjugation of inhaled corticosteroids within the lung may allow prolonged duration of effect, enabling once-daily administration. Pharmacodynamic and pharmacokinetic principles probably do not play a role in describing upper airway adverse effects occurring with inhaled corticosteroids. These are probably also determined by intrinsic properties of the drug and deposition characteristics. However, pharmacodynamic and pharmacokinetic principles seem to be important in addressing systemic safety concerns with inhaled corticosteroids. Those inhaled corticosteroids with a longer serum half-life, especially if they have higher affinity for the corticosteroid receptor, may be associated with greater systemic effects. A new pharmacokinetic concept suggests that increased protein binding within the systemic circulation and high systemic clearance of an inhaled corticosteroid may reduce the risk for systemic effects. These new pharmacodynamic and pharmacokinetic concepts provide a useful framework for identifying the characteristics of an inhaled corticosteroid with an improved benefit-to-risk profile. Increased lung deposition and reduced deposition in the upper airway should result in an inhaled corticosteroid with favorable clinical efficacy and a decreased risk for topical upper airway adverse effects. An inhaled corticosteroid with high plasma protein binding and rapid clearance might pose much less risk for systemic adverse effects than currently available drugs in this class.

摘要

吸入性糖皮质激素在控制气道炎症方面有效。它们的抗炎作用主要是局部性的,作用于气道内的药物沉积部位。因此,依赖于测量药物血药浓度的传统药效学和药代动力学概念,在评估局部作用的吸入性糖皮质激素疗效方面适用性有限。影响吸入性糖皮质激素疗效的重要因素有:(i)药物的内在特性,特别是它们对糖皮质激素受体的亲和力;以及(ii)药物制剂沉积特性这一较新的药效学概念。小颗粒制剂,尤其是那些用新型氢氟烷烃推进剂开发的定量吸入器中的制剂,在肺部的沉积程度要大得多,因此可能具有更好的临床疗效。吸入性糖皮质激素在肺内的脂质结合可能使作用持续时间延长,从而实现每日一次给药。药效学和药代动力学原理可能在描述吸入性糖皮质激素引起的上呼吸道不良反应方面不起作用。这些不良反应可能也由药物的内在特性和沉积特性决定。然而,药效学和药代动力学原理在解决吸入性糖皮质激素的全身安全性问题方面似乎很重要。那些血清半衰期较长的吸入性糖皮质激素,特别是如果它们对糖皮质激素受体具有更高的亲和力,可能会产生更大的全身效应。一种新的药代动力学概念表明,吸入性糖皮质激素在体循环中蛋白结合增加和全身清除率高可能会降低全身效应的风险。这些新的药效学和药代动力学概念为识别具有改善的效益风险比的吸入性糖皮质激素的特性提供了一个有用的框架。肺部沉积增加和上呼吸道沉积减少应会产生一种具有良好临床疗效且上呼吸道局部不良反应风险降低的吸入性糖皮质激素。与该类目前可用的药物相比,一种具有高血浆蛋白结合率和快速清除率的吸入性糖皮质激素可能引起全身不良反应的风险要小得多。

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