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American journal of veterinary research2023; 1-6; doi: 10.2460/ajvr.23.04.0076

Botulinum neurotoxin type A does not exert concentration-dependent effects on equine articular cartilage in vitro.

Abstract: To determine whether Botulinum neurotoxin type A (BoNT-A) ameliorates the effects of interleukin 1 (IL-1) on equine articular cartilage, or exerts negative effects on normal equine articular cartilage homeostasis in vitro. Methods: Articular cartilage explants from 6 healthy femoropatellar joints of 3 adult horses. Methods: Explants were allocated to the IL-1 challenged or unchallenged group, then exposed to 1 of 6 concentrations of BoNT-A (0, 1, 10, 50, 100, or 500 pg/mL) for 96 hours. To assess BoNT-A's effects on inflammation, prostaglandin E2 (PGE2) was measured in media via ELISA. Matrix degradation was determined as the percentage of sulfated glycosaminoglycans (sGAG) released from explants via dimethylmethylene blue assay. Aggrecan synthesis was estimated using CS846 ELISA and collagen type II degradation was estimated using C2C ELISA on media. Chondrocyte apoptosis was assessed via in-situ TUNEL assay. Generalized linear mixed models were fitted to determine treatment effects using α = 0.05. Results: The challenge with IL-1 resulted in increased concentrations of PGE2 and CS846 in media and increased release of sGAG from explants. BoNT-A did not significantly impact PGE2 or CS846 concentration in media, percentage of sGAG released, or chondrocyte apoptosis in IL-1 challenged or unchallenged cartilage explants. The concentration of C2C in media was below the quantifiable limit of the ELISA in all samples. Conclusions: BoNT-A did not show chondroprotective effects or have negative effects on cartilage homeostasis in vitro at the concentrations tested. While chondroprotective effects were not observed, BoNT-A may be safe for intraarticular use. In vivo testing is warranted before clinical use.
Publication Date: 2023-07-18 PubMed ID: 37442543DOI: 10.2460/ajvr.23.04.0076Google Scholar: Lookup
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  • Journal Article

Summary

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The study investigates the effects of Botulinum neurotoxin type A (BoNT-A) on equine articular cartilage, both in the presence and absence of interleukin 1 (IL-1). It concludes that BoNT-A does not have significant chondroprotective or negative effects on cartilage homeostasis in vitro, and further in vivo testing is warranted.

Objective

  • The study aimed to determine whether BoNT-A can ameliorate the effects of IL-1 on horse cartilage or if it negatively affects normal cartilage homeostasis in vitro.

Methods

  • Articular cartilage samples were taken from 6 healthy joints of 3 adult horses.
  • Explants were challenged with IL-1 or left unchallenged, then exposed to 6 concentrations of BoNT-A for 96 hours.
  • Inflammation was assessed by measuring PGE2 in media via ELISA.
  • Matrix degradation was determined through the percentage of sGAG released.
  • Aggrecan synthesis and collagen type II degradation were estimated using CS846 and C2C ELISA, respectively.
  • Chondrocyte apoptosis was assessed using the TUNEL assay.

Results

  • IL-1 challenge increased concentrations of PGE2 and CS846 and the release of sGAG from explants.
  • BoNT-A did not significantly impact these factors in either challenged or unchallenged cartilage explants.
  • C2C concentration in media was below the quantifiable limit in all samples.

Conclusions

  • The study concluded that BoNT-A did not show chondroprotective effects or negative impacts on cartilage homeostasis in vitro at the tested concentrations.
  • While chondroprotective effects were not observed, BoNT-A may be safe for intra-articular use, and in vivo testing is recommended before clinical use.

Cite This Article

APA
McCarthy MB, Duesterdieck-Zellmer KF, Larson MK. (2023). Botulinum neurotoxin type A does not exert concentration-dependent effects on equine articular cartilage in vitro. Am J Vet Res, 1-6. https://doi.org/10.2460/ajvr.23.04.0076

Publication

ISSN: 1943-5681
NlmUniqueID: 0375011
Country: United States
Language: English
Pages: 1-6

Researcher Affiliations

McCarthy, Meghan B
    Duesterdieck-Zellmer, Katja F
      Larson, Maureen K

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