Literature DB >> 30874257

Engineering an immunomodulatory drug-eluting stent to treat laryngotracheal stenosis.

Madhavi Duvvuri1, Kevin Motz, Michael Murphy, Michael Feeley, Dacheng Ding, Andrew Lee, Jennifer H Elisseeff, Alexander T Hillel.   

Abstract

OBJECTIVE: Develop a drug-eluting stent construct with a reliable drug-release profile and adequate mechanically stability for a trial in a small animal model of laryngotracheal stenosis (LTS), a debilitating pathologic narrowing of the airway leading to significant shortness of breath.
METHODS: Biodegradable, biocompatible stents containing 1.0% rapamycin made of PLLA-PCL (70% Poly-l-Lactide and 30% Polycaprolactone blend) and 50 : 50 PDLGA (Poly(dl-lactide-co-glycolide)) were compared. Mechanical strength testing and drug elution rates using high performance liquid chromatography analysis (HPLC) was assessed. Next, efficacy of stent elution on LTS derived scar fibroblasts. Finally, stents were placed in situ in an LTS mouse model.
RESULTS: The PLLA-PCL stent construct exhibited greater mechanical strength compared to the PDLGA stent over a 4-week period (Young's Modulus (PLLA-PCL) = 13.82; Young's Modulus (PDLGA) = 4.015). Moreover, the PLLA-PCL stent showed a reliable rapamycin release profile for 6 weeks (30% elution for PLLA-PCL stents compared to <1% elution for PDLGA). Collagen 1 (p < 0.05) and fibroblast cell proliferation were decreased in vitro when treated with the rapamycin stent. In vivo, the rapamycin stent reduced lamina propria thickness (p < 0.05) and collagen 1(p < 0.05), collagen 3, TGF-B (p < 0.05) and a-SMA (p < 0.05).
CONCLUSIONS: The PLLA-PCL construct demonstrated superior mechanical strength and greater drug elution compared to PDLGA stents. We demonstrated the feasibility of testing this drug-eluting stent in vivo, showing that the rapamycin-eluting stent treats fibrosis. To our knowledge this is the first study to deploy a drug-eluting stent to treat tracheal pathology in an animal model. Optimization of a rapamycin-eluting PLLA-PCL stent for translational investigation will lead to improved treatment strategies of LTS.

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Year:  2019        PMID: 30874257      PMCID: PMC6478537          DOI: 10.1039/c8bm01623b

Source DB:  PubMed          Journal:  Biomater Sci        ISSN: 2047-4830            Impact factor:   6.843


  26 in total

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Review 3.  The mammalian target of rapamycin: linking T cell differentiation, function, and metabolism.

Authors:  Jonathan D Powell; Greg M Delgoffe
Journal:  Immunity       Date:  2010-09-24       Impact factor: 31.745

4.  Prognostic factors in laryngotracheal injury following intubation and/or tracheotomy in ICU patients.

Authors:  E Esteller-Moré; J Ibañez; E Matiñó; J M Ademà; M Nolla; I M Quer
Journal:  Eur Arch Otorhinolaryngol       Date:  2005-10-29       Impact factor: 2.503

5.  Investigation of PLLA/PCL blends and paclitaxel release profiles.

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6.  A novel bioabsorbable drug-eluting tracheal stent.

Authors:  G H Zhu; Anthony H C Ng; Subbu S Venkatraman; Freddy Y C Boey; Amilia L Y Wee; Scott L Trasti; Lynne Hsueh Yee Lim
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7.  Photoactivated composite biomaterial for soft tissue restoration in rodents and in humans.

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8.  Modern management of laryngotracheal stenosis.

Authors:  Heather C Herrington; Stephen M Weber; Peter E Andersen
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9.  Use of internal bioabsorbable PLGA "finger-type" stents in a rabbit tracheal reconstruction model.

Authors:  T C Robey; T Välimaa; H S Murphy; P Tôrmâlâ; D J Mooney; R A Weatherly
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Review 3.  A narrative review of progress in airway stents.

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4.  Design of a Biocompatible Drug-Eluting Tracheal Stent in Mice with Laryngotracheal Stenosis.

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5.  Glutamine Inhibition Reduces Iatrogenic Laryngotracheal Stenosis.

Authors:  Hsiu-Wen Tsai; Ioan Lina; Kevin M Motz; Liam Chung; Dacheng Ding; Michael K Murphy; Michael Feeley; Jennifer H Elisseeff; Alexander T Hillel
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Review 7.  Molecular Mechanisms and Physiological Changes behind Benign Tracheal and Subglottic Stenosis in Adults.

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Review 8.  Inflammatory pathways in the pathogenesis of iatrogenic laryngotracheal stenosis: what do we know?

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