Literature DB >> 23932897

Airway drug pharmacokinetics via analysis of exhaled breath condensate.

Charles R Esther1, Richard C Boucher2, M Ross Johnson3, John H Ansede3, Karl H Donn3, Thomas G O'Riordan4, Andrew J Ghio5, Andrew J Hirsh3.   

Abstract

Although the airway surface is the anatomic target for many lung disease therapies, measuring drug concentrations and activities on these surfaces poses considerable challenges. We tested whether mass spectrometric analysis of exhaled breath condensate (EBC) could be utilized to non-invasively measure airway drug pharmacokinetics and predicted pharmacological activities. Mass spectrometric methods were developed to detect a novel epithelial sodium channel blocker (GS-9411/P-680), two metabolites, a chemically related internal standard, plus naturally occurring solutes including urea as a dilution marker. These methods were then applied to EBC and serum collected from four (Floridian) sheep before, during and after inhalation of nebulized GS-9411/P-680. Electrolyte content of EBC and serum was also assessed as a potential pharmacodynamic marker of drug activity. Airway surface concentrations of drug, metabolites, and electrolytes were calculated from EBC measures using EBC:serum urea based dilution factors. GS-9411/P-680 and its metabolites were quantifiable in the sheep EBC, with peak airway concentrations between 1.9 and 3.4 μM measured 1 h after inhalation. In serum, only Metabolite #1 was quantifiable, with peak concentrations ∼60-fold lower than those in the airway (45 nM at 1 h). EBC electrolyte concentrations suggested a pharmacological effect; but this effect was not statistical significant. Analysis of EBC collected during an inhalation drug study provided a method for quantification of airway drug and metabolites via mass spectrometry. Application of this methodology could provide an important tool in development and testing of drugs for airways diseases.
Copyright © 2013 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  EBC; Exhaled breath condensate; ICP-MS; ICP-OES; K; LC-MS/MS; MS; Na; Pharmacokinetics; SRM; Sheep; Sodium channel; Urea; exhaled breath condensate; inductively coupled plasma-mass spectrography; inductively coupled plasma-optical emission spectrography; liquid chromatography-tandem mass spectrometry; mass spectrometry; potassium; selected reaction monitoring; sodium

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Year:  2013        PMID: 23932897      PMCID: PMC3947122          DOI: 10.1016/j.pupt.2013.07.009

Source DB:  PubMed          Journal:  Pulm Pharmacol Ther        ISSN: 1094-5539            Impact factor:   3.410


  22 in total

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9.  The nature of small-airway obstruction in chronic obstructive pulmonary disease.

Authors:  James C Hogg; Fanny Chu; Soraya Utokaparch; Ryan Woods; W Mark Elliott; Liliana Buzatu; Ruben M Cherniack; Robert M Rogers; Frank C Sciurba; Harvey O Coxson; Peter D Paré
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3.  Potentiator ivacaftor abrogates pharmacological correction of ΔF508 CFTR in cystic fibrosis.

Authors:  Deborah M Cholon; Nancy L Quinney; M Leslie Fulcher; Charles R Esther; Jhuma Das; Nikolay V Dokholyan; Scott H Randell; Richard C Boucher; Martina Gentzsch
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Review 4.  Exhaled Breath Condensate: Technical and Diagnostic Aspects.

Authors:  Efstathia M Konstantinidi; Andreas S Lappas; Anna S Tzortzi; Panagiotis K Behrakis
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  5 in total

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