Intra-articular injection of triamcinolone acetonide releasing biomaterial microspheres inhibits pain and inflammation in an acute arthritis model.


Journal

Drug delivery
ISSN: 1521-0464
Titre abrégé: Drug Deliv
Pays: England
ID NLM: 9417471

Informations de publication

Date de publication:
Dec 2019
Historique:
entrez: 8 3 2019
pubmed: 8 3 2019
medline: 23 7 2019
Statut: ppublish

Résumé

Inflammation of the synovium and joint capsule is a main driver of pain in an osteoarthritic (OA) joint. Triamcinolone acetonide (TAA) is a classical corticosteroid that reduces synovitis and alleviates pain, albeit transiently. Biomaterial-based local TAA release may prolong the suppression of pain without the need for multiple injections. Polylactic-co-glycolic acid (PLGA) formulations of TAA prolong OA pain relief to a limited extent. A novel polyesteramide (PEA) microsphere platform allows for extended release in the OA joint for over 3 months. To evaluate their effect on pain and inflammation, TAA-loaded microspheres were intra-articularly delivered to the knee joint in a rat model of acute arthritis induced by intra-articular injection of streptococcal cell wall peptidoglycan-polysaccharide (PGPS) and subsequent flare-ups by intravenous PGPS injections. PEA-loaded microspheres were benchmarked with TAA-loaded PLGA microspheres and bolus TAA injection. TAA treatments were injected intra-articularly before the first induced flare-up. TAA-loaded PEA and PLGA microspheres reduced joint swelling and signs of pain-like behavior over the entire study period, as assessed by weight bearing and referred mechanical hypersensitivity, whereas bolus suspension was effective for a shorter time period. TAA-loaded PEA microspheres reduced lameness to a greater extent than TAA-loaded PLGA microspheres. In conclusion, a single intra-articular injection of TAA-loaded PEA microspheres reduced joint swelling and induced longer pain relief compared to bolus injection. Hence relief of inflammation and pain by PEA-based delivery of TAA may prove to be effective and durable.

Identifiants

pubmed: 30843733
pii: 10.1080/10717544.2019.1568625
pmc: PMC6407600

Substances chimiques

Acrylic Resins 0
Biocompatible Materials 0
poly(ethylacrylate) 0
Polylactic Acid-Polyglycolic Acid Copolymer 1SIA8062RS
Triamcinolone Acetonide F446C597KA

Types de publication

Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

226-236

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Auteurs

Imke Rudnik-Jansen (I)

a Department of Orthopedics , University Medical Center Utrecht , Utrecht , the Netherlands.

Karin Schrijver (K)

a Department of Orthopedics , University Medical Center Utrecht , Utrecht , the Netherlands.

Nina Woike (N)

b DSM Biomedical B.V , Geleen , The Netherlands.

Anna Tellegen (A)

c Department of Clinical Sciences of Companion Animals , Utrecht University , Utrecht , the Netherlands.

Sabine Versteeg (S)

d Laboratory of Translational Immunology , University Medical Center Utrecht, Utrecht University , Utrecht , the Netherlands.

Pieter Emans (P)

e Department of Orthopedics , Maastricht University Medical Center Utrecht , Utrecht , the Netherlands.

George Mihov (G)

b DSM Biomedical B.V , Geleen , The Netherlands.

Jens Thies (J)

b DSM Biomedical B.V , Geleen , The Netherlands.

Niels Eijkelkamp (N)

d Laboratory of Translational Immunology , University Medical Center Utrecht, Utrecht University , Utrecht , the Netherlands.

Marianna Tryfonidou (M)

c Department of Clinical Sciences of Companion Animals , Utrecht University , Utrecht , the Netherlands.

Laura Creemers (L)

a Department of Orthopedics , University Medical Center Utrecht , Utrecht , the Netherlands.

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Classifications MeSH