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  5. Intra-articular delivery of a nanocomplex comprising salmon calcitonin, hyaluronic acid, and chitosan using an equine model of joint inflammation
 
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Intra-articular delivery of a nanocomplex comprising salmon calcitonin, hyaluronic acid, and chitosan using an equine model of joint inflammation

Author(s)
Sladek, Svenja  
Kearney, Clodagh  
Crean, Daniel  
Brama, Pieter A. J.  
Tajber, Lidia  
Fawcett, Karolina  
Labberte, Margot C.  
Leggett, Bernadette  
Brayden, David James  
Uri
http://hdl.handle.net/10197/10032
Date Issued
2018-10
Date Available
2019-04-18T08:45:37Z
Abstract
Polyelectrolyte nanoparticle constructs (NPs) comprising salmon calcitonin (sCT), chitosan (CS), and hyaluronic acid (HA) were previously established as having anti-inflammatory potential when injected via the intra-articular (i.a.) route to a mouse model. We attempted to translate the formulation to a large animal model, the lipopolysaccharide (LPS)-stimulated equine model of joint inflammation. The aim was to manufacture under aseptic conditions to produce sterile pyrogen-free NPs, to confirm physicochemical characteristics, and to test toxicity and efficacy in a pilot study. NP dispersions were successfully formulated using pharmaceutical-grade source materials and were aseptically manufactured under GMP-simulated conditions in a grade A modular aseptic processing workstation. The NP formulation had no detectable pathogen or endotoxin contamination. NPs were then tested versus a lactated Ringer’s solution control following single i.a. injections to the radiocarpal joints of two groups of four horses pre-treated with LPS, followed by arthrocentesis at set intervals over 1 week. There was no evidence of treatment-related toxicity over the period. While there were no differences between clinical read-outs of the NP and the control, two synovial fluid-derived biomarkers associated with cartilage turnover revealed a beneficial effect of NPs. In conclusion, NPs comprising well-known materials were manufactured for an equine i.a.-injectable pilot study and yielded no NP-attributable toxicity. Evidence of NP-associated benefit at the level of secondary endpoints was detected as a result of decreases in synovial fluid inflammatory biomarkers.
Sponsorship
European Commission
Science Foundation Ireland
Other Sponsorship
Wellcome Trust Institutional Strategic Support Fund Clinician Stimulus Scheme (CK)
SFI Synthesis and Solid State Pharmaceutical Centre
Type of Material
Journal Article
Publisher
Springer
Journal
Drug Delivery and Translational Research
Volume
8
Issue
5
Start Page
1421
End Page
1435
Copyright (Published Version)
2018 Controlled Release Society
Subjects

Salmon calcitonin

Hyaluronic acid

Chitosan

Joint inflammation

Synovitis

Nanomedicine

Large animal models

DOI
10.1007/s13346-018-0557-x
Language
English
Status of Item
Peer reviewed
ISSN
2190-3948
This item is made available under a Creative Commons License
https://creativecommons.org/licenses/by-nc-nd/3.0/ie/
File(s)
No Thumbnail Available
Name

Sladek RMS.docx

Size

1.39 MB

Format

Unknown

Checksum (MD5)

29d6ec0819a1716b1c577f5dca86c83d

Owning collection
Veterinary Medicine Research Collection
Mapped collections
Conway Institute Research Collection

Item descriptive metadata is released under a CC-0 (public domain) license: https://creativecommons.org/public-domain/cc0/.
All other content is subject to copyright.

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