Human Pharmacokinetics/Pharmacodynamics of an Interleukin-4 and Interleukin-13 Dual Antagonist in Asthma

Pitrakinra, a 15‐kDa recombinant human interleukin‐4 mutein, targets allergic Th2 inflammation by competitively binding to interleukin‐4 receptor alpha to interfere with interleukin‐4 and interleukin‐13 action. The authors characterized pitrakinra pharmacokinetics using data from 96 atopic patients,...

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Bibliographic Details
Published in:Journal of clinical pharmacology 2009-09, Vol.49 (9), p.1025-1036
Main Authors: Getz, Elise Burmeister, Fisher, Dennis M., Fuller, Rick
Format: Article
Language:English
Subjects:
Administration, Inhalation
Adolescent
Adult
Anti-Asthmatic Agents - administration & dosage
Anti-Asthmatic Agents - pharmacokinetics
Anti-Asthmatic Agents - pharmacology
Asthma
Asthma - drug therapy
Asthma - physiopathology
Biological Availability
Clinical Trials, Phase I as Topic
Clinical Trials, Phase II as Topic
Female
Half-Life
Humans
Injections, Subcutaneous
interleukin-13
Interleukin-13 - antagonists & inhibitors
interleukin-4
Interleukin-4 - antagonists & inhibitors
Lung - metabolism
Male
Middle Aged
Models, Biological
pharmacokinetics
pitrakinra
Young Adult
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Summary:Pitrakinra, a 15‐kDa recombinant human interleukin‐4 mutein, targets allergic Th2 inflammation by competitively binding to interleukin‐4 receptor alpha to interfere with interleukin‐4 and interleukin‐13 action. The authors characterized pitrakinra pharmacokinetics using data from 96 atopic patients, then compared pharmacokinetics with pharmacological response in asthma following subcutaneous versus inhalation dosing. A 1‐compartment systemic model with site‐specific absorption describes pitrakinra pharmacokinetics following subcutaneous, nebulization, and inhalation powder delivery. Typical CL/F and V/F, referenced to subcutaneous administration, are 15.5 L/h and 67.5 L, yielding a 3.0‐hour half‐life of plasma decline. Absorption into the blood (half‐life ≤1.0 hour, lag ≤18 minutes) is more rapid than elimination. Relative to subcutaneous injection, systemic availability of the first inhaled dose is ≤3%. Subcutaneous injection produced variable efficacy despite high systemic exposure, suggesting inadequate exposure at the site of action in some participants. Inhalation produced consistent pharmacodynamic response despite low systemic exposure. The lung appears as the primary site of pitrakinra's antiasthmatic action, supporting direct administration to the lung for the treatment of asthma.
ISSN:0091-2700
1552-4604
DOI:10.1177/0091270009341183