Intrapulmonary pharmacokinetics of antibacterial agents: implications for therapeutics.

Loretta M Chiu, Guy W Amsden
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引用次数: 8

Abstract

The idea of studying the pharmacokinetics and pharmacodynamics of antibacterials in order to predict their efficacy has long been of interest. Traditionally, serum drug concentrations have been evaluated against the minimum inhibitory concentration (MIC) of a given pathogen; however, infection site-specific data continue to gain interest from clinicians. Despite methodological limitations, progress in techniques has improved the clinical significance of data generated. Rather than using tissue homogenates which fail to differentiate between interstitial and intracellular concentrations, newer collection techniques focus on sampling of matrices that allow for this differentiation. These collection techniques now allow one to accurately describe beta-lactam and aminoglycoside interstitial penetrations, as well as, the interstitial and phagocytic concentrations of macrolides and fluoroquinolones. By using these specific data and the MICs of infecting pathogens, it is hoped that conclusions can be drawn by a clinician as to the appropriateness of the choice of an antibacterial.

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抗菌药物的肺内药代动力学:治疗学意义。
研究抗菌药物的药代动力学和药效学以预测其疗效的想法长期以来一直引起人们的兴趣。传统上,血清药物浓度是根据给定病原体的最低抑制浓度(MIC)来评估的;然而,感染部位特异性数据继续引起临床医生的兴趣。尽管有方法学上的局限性,但技术的进步提高了所生成数据的临床意义。而不是使用组织匀浆,不能区分间质和细胞内浓度,较新的收集技术侧重于基质的采样,允许这种分化。这些收集技术现在允许人们准确地描述-内酰胺和氨基糖苷间质渗透,以及大环内酯类和氟喹诺酮类药物的间质和吞噬浓度。通过使用这些特定的数据和感染病原体的mic,希望临床医生可以得出结论,选择适当的抗菌药物。
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