AI Article Synopsis

  • Human plasma-derived 1-antitrypsin (AAT) is used to treat emphysema in patients with a genetic deficiency, and inhalation may improve the treatment's efficacy and convenience compared to intravenous infusion.
  • This study examined the effectiveness of delivering recombinant AAT (rAAT) directly to the lungs of mice via intratracheal administration by assessing its distribution and pharmacokinetics.
  • Results showed that rAAT effectively reached areas with neutrophil elastase in the lungs, providing data that may help predict appropriate dosing for human inhalation therapies.

Article Abstract

Human plasma-derived 1-antitrypsin (AAT) delivered by intravenous infusion is used as augmentation therapy in patients with emphysema who have a genetic mutation resulting in deficiency of AAT. Inhalation is an alternative route of administration that can potentially increase the efficacy and convenience of treatment. This study was conducted to determine whether delivery to the lungs, initially via the intratracheal (IT) route of administration, would deliver efficacious levels of a recombinant AAT (rAAT) to the site of action in the lungs in mice. I-radiolabeled rAAT, fluorophore-conjugated rAAT (rAAT-Alexa488), and NE680 (neutrophil elastase 680, a silent fluorescent substrate of neutrophil elastase which fluoresces in the near-infrared range upon activation by neutrophil elastase) were used to characterize the pharmacokinetics and tissue distribution profile, distribution of rAAT within the lung, and efficacy of rAAT to inhibit neutrophil elastase at the site of action, respectively. The study has demonstrated that rAAT was able to gain access to locations where neutrophil elastase was localized. The histochemical quantification of rAAT activity relative to dose at the site of action provided here will improve confidence in predicting the human dose via the inhalation route.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5168502PMC
http://dx.doi.org/10.1155/2016/5768312DOI Listing

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