Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model

Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model

Intravenous (IV) topotecan is approved for the treatment of various malignancies including lung cancer but its clinical use is greatly undermined by severe hematopoietic toxicity. We hypothesized that inhalation delivery of topotecan would increase local exposure and efficacy against lung cancer whi...

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Main Authors: Philip J. Kuehl, Marcie J. Grimes, Devon Dubose, Michael Burke, David A. Revelli, Andrew P. Gigliotti, Steven A. Belinsky, Mathewos Tessema
Format: Article
Language:English
Published: Taylor & Francis Group 2018-01-01
Series:Drug Delivery
Subjects:
topotecan
inhalation
lung cancer
aerosol
dry powder
Online Access:http://dx.doi.org/10.1080/10717544.2018.1469688
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spelling doaj-3849580988424c208877112a36103a872020-11-25T03:13:32ZengTaylor & Francis GroupDrug Delivery1071-75441521-04642018-01-012511127113610.1080/10717544.2018.14696881469688Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical modelPhilip J. Kuehl0Marcie J. Grimes1Devon Dubose2Michael Burke3David A. Revelli4Andrew P. Gigliotti5Steven A. Belinsky6Mathewos Tessema7Lovelace BiomedicalLovelace Respiratory Research InstituteLonza-Bend Research InstituteLonza-Bend Research InstituteLovelace BiomedicalLovelace BiomedicalLovelace Respiratory Research InstituteLovelace Respiratory Research InstituteIntravenous (IV) topotecan is approved for the treatment of various malignancies including lung cancer but its clinical use is greatly undermined by severe hematopoietic toxicity. We hypothesized that inhalation delivery of topotecan would increase local exposure and efficacy against lung cancer while reducing systemic exposure and toxicity. These hypotheses were tested in a preclinical setting using a novel inhalable formulation of topotecan against the standard IV dose. Respirable dry-powder of topotecan was manufactured through spray-drying technology and the pharmacokinetics of 0.14 and 0.79 mg/kg inhalation doses were compared with 0.7 mg/kg IV dose. The efficacy of four weekly treatments with 1 mg/kg inhaled vs. 2 mg/kg IV topotecan were compared to untreated control using an established orthotopic lung cancer model for a fast (H1975) and moderately growing (A549) human lung tumors in the nude rat. Inhalation delivery increased topotecan exposure of lung tissue by approximately 30-fold, lung and plasma half-life by 5- and 4-folds, respectively, and reduced the maximum plasma concentration by 2-fold than the comparable IV dose. Inhaled topotecan improved the survival of rats with the fast-growing lung tumors from 7 to 80% and reduced the tumor burden of the moderately-growing lung tumors over 5- and 10-folds, respectively, than the 2-times higher IV topotecan and untreated control (p < .00001). These results indicate that inhalation delivery increases topotecan exposure of lung tissue and improves its efficacy against lung cancer while also lowering the effective dose and maximum systemic concentration that is responsible for its dose-limiting toxicity.http://dx.doi.org/10.1080/10717544.2018.1469688topotecaninhalationlung canceraerosoldry powder
collection DOAJ
language English
format Article
sources DOAJ
author Philip J. Kuehl
Marcie J. Grimes
Devon Dubose
Michael Burke
David A. Revelli
Andrew P. Gigliotti
Steven A. Belinsky
Mathewos Tessema
spellingShingle Philip J. Kuehl
Marcie J. Grimes
Devon Dubose
Michael Burke
David A. Revelli
Andrew P. Gigliotti
Steven A. Belinsky
Mathewos Tessema
Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
Drug Delivery
topotecan
inhalation
lung cancer
aerosol
dry powder
author_facet Philip J. Kuehl
Marcie J. Grimes
Devon Dubose
Michael Burke
David A. Revelli
Andrew P. Gigliotti
Steven A. Belinsky
Mathewos Tessema
author_sort Philip J. Kuehl
title Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
title_short Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
title_full Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
title_fullStr Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
title_full_unstemmed Inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
title_sort inhalation delivery of topotecan is superior to intravenous exposure for suppressing lung cancer in a preclinical model
publisher Taylor & Francis Group
series Drug Delivery
issn 1071-7544
1521-0464
publishDate 2018-01-01
description Intravenous (IV) topotecan is approved for the treatment of various malignancies including lung cancer but its clinical use is greatly undermined by severe hematopoietic toxicity. We hypothesized that inhalation delivery of topotecan would increase local exposure and efficacy against lung cancer while reducing systemic exposure and toxicity. These hypotheses were tested in a preclinical setting using a novel inhalable formulation of topotecan against the standard IV dose. Respirable dry-powder of topotecan was manufactured through spray-drying technology and the pharmacokinetics of 0.14 and 0.79 mg/kg inhalation doses were compared with 0.7 mg/kg IV dose. The efficacy of four weekly treatments with 1 mg/kg inhaled vs. 2 mg/kg IV topotecan were compared to untreated control using an established orthotopic lung cancer model for a fast (H1975) and moderately growing (A549) human lung tumors in the nude rat. Inhalation delivery increased topotecan exposure of lung tissue by approximately 30-fold, lung and plasma half-life by 5- and 4-folds, respectively, and reduced the maximum plasma concentration by 2-fold than the comparable IV dose. Inhaled topotecan improved the survival of rats with the fast-growing lung tumors from 7 to 80% and reduced the tumor burden of the moderately-growing lung tumors over 5- and 10-folds, respectively, than the 2-times higher IV topotecan and untreated control (p < .00001). These results indicate that inhalation delivery increases topotecan exposure of lung tissue and improves its efficacy against lung cancer while also lowering the effective dose and maximum systemic concentration that is responsible for its dose-limiting toxicity.
topic topotecan
inhalation
lung cancer
aerosol
dry powder
url http://dx.doi.org/10.1080/10717544.2018.1469688
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