Local and systemic inflammatory and immunologic reactions to cyathostomin larvicidal therapy in horses.
Abstract: Encysted cyathostomin larvae are ubiquitous in grazing horses. Arrested development occurs in this population and can lead to an accumulation of encysted larvae. Large numbers of tissue larvae place the horse at risk for developing larval cyathostominosis. This disease complex is caused by mass emergence of these larvae and is characterized by a generalized acute typhlocolitis and manifests itself as a profuse protein-losing watery diarrhea with a reported case-fatality rate of about 50%. Two anthelmintic formulations have a label claim for larvicidal therapy of these encysted stages; moxidectin and a five-day regimen of fenbendazole. There is limited knowledge about inflammatory and immunologic reactions to larvicidal therapy. This study was designed to evaluate blood acute phase reactants as well as gene expression of pro-inflammatory cytokines, both locally in the large intestinal walls and systemically. Further, mucosal tissue samples were evaluated histopathologically as well as analyzed for gene expression of pro- and anti-inflammatory cytokines, cluster of differentiation (CD) cell surface proteins, and select transcription factors. Eighteen juvenile horses with naturally acquired cyathostomin infections were randomly assigned to three treatment groups; one group served as untreated controls (Group 1), one received a five-day regimen of fenbendazole (10mg/kg) (Group 2), and one group received moxidectin (0.4mg/kg) (Group 3). Horses were treated on day 0 and euthanatized on days 18-20. Serum and whole blood samples were collected on days 0, 5, and 18. All horses underwent necropsy with collection of tissue samples from the ventral colon and cecum. Acute phase reactants measured included serum amyloid A, iron and fibrinogen, and the cytokines evaluated included interferon γ, tumor necrosis factor α, transforming growth factor (TGF)-β, and interleukins 1β, 4, 5, 6, and 10. Transcription factors evaluated were FoxP3, GATA3 and tBet, and CD markers included CD163, CD3z, CD4, CD40, and CD8b. Histopathology revealed an inflammatory reaction with higher levels of lymphocytes, T cells, B cells, eosinophils and fibrous tissue in the moxidectin-treated group compared to controls or horses treated with fenbendazole. No apparent systemic reactions were observed. Expression of IL-5 and TGF-β in intestinal tissues was significantly lower in Group 3 compared to Group 1. This study revealed a subtle inflammatory reaction to moxidectin, which is unlikely to cause clinical issues.
Copyright © 2015 Elsevier B.V. All rights reserved.
Publication Date: 2015-09-25 PubMed ID: 26429413DOI: 10.1016/j.vetimm.2015.09.009Google Scholar: Lookup
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- Journal Article
- Randomized Controlled Trial
Summary
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This study investigates the local and systemic inflammatory and immunologic responses in horses following treatment for cyathostomin larvicidal infection. The research compares the effects of two common anthelmintic treatments, moxidectin and fenbendazole, and found that moxidectin treatment resulted in an inflammatory reaction, but one that is unlikely to cause clinical issues.
Introduction to the Study
- The focus of this research is to understand the inflammatory and immunologic reactions in horses after treatment for cyathostomin larvicidal infection, a common condition caused by the buildup of encysted larvae in grazing horses, which can lead to a severe disease known as larval cyathostominosis.
- Two commonly used treatments for this infection are moxidectin and fenbendazole, but our understanding about how these drugs cause inflammatory and immunologic reactions remains incomplete.
Study Design and Methods
- Eighteen juvenile horses with naturally acquired infections were grouped into three. The first group was untreated, the second received fenbendazole, and the third received moxidectin.
- The horses were treated on day 0 and were euthanized on days 18-20 for necropsy.
- During the study, blood and tissue samples were collected to measure acute phase reactants, evaluate the gene expression of cytokines, cluster of differentiation (CD) cell surface proteins, and transcription factors.
Findings
- The histopathological examination found evidence of an inflammatory reaction in the moxidectin-treated group in the form of higher levels of lymphocytes, T cells, B cells, eosinophils and fibrous tissue. No such reaction was observed in the fenbendazole-treated group or control (untreated) group.
- However, the inflammatory reaction triggered by moxidectin was found to be subtle and it’s unlikely to lead to clinical problems.
- No significant systemic reactions were detected post-treatment.
- The gene expression of interleukin-5 (IL-5) and transforming growth factor-beta (TGF-β) in the intestinal tissues was significantly lower in the moxidectin-treated group compared to the untreated groups.
Conclusion
- Although the study revealed moxidectin triggers a mild inflammatory reaction in horses, the reaction is unlikely to result in clinical complications.
- The study contributes valuable knowledge to our understanding of the biological responses in horses following larvicidal therapy for cyathostomin infection.
Cite This Article
APA
Nielsen MK, Loynachan AT, Jacobsen S, Stewart JC, Reinemeyer CR, Horohov DW.
(2015).
Local and systemic inflammatory and immunologic reactions to cyathostomin larvicidal therapy in horses.
Vet Immunol Immunopathol, 168(3-4), 203-210.
https://doi.org/10.1016/j.vetimm.2015.09.009 Publication
Researcher Affiliations
- Maxwell H. Gluck Equine Research Center, Department of Veterinary Science, University of Kentucky, Lexington, KY, USA. Electronic address: martin.nielsen@uky.edu.
- Veterinary Diagnostic Laboratory, Department of Veterinary Science, University of Kentucky, Lexington, KY, USA.
- Department of Large Animal Sciences, University of Copenhagen, Taastrup, Denmark.
- Maxwell H. Gluck Equine Research Center, Department of Veterinary Science, University of Kentucky, Lexington, KY, USA.
- East Tennessee Clinical Research, Inc., Rockwood, TN, USA.
- Maxwell H. Gluck Equine Research Center, Department of Veterinary Science, University of Kentucky, Lexington, KY, USA.
MeSH Terms
- Animals
- Anthelmintics / adverse effects
- Anthelmintics / therapeutic use
- Biomarkers / blood
- Cecum / drug effects
- Cecum / pathology
- Colon / drug effects
- Colon / pathology
- Cytokines / blood
- Cytokines / genetics
- Cytokines / metabolism
- Fenbendazole / adverse effects
- Fenbendazole / therapeutic use
- Gene Expression Regulation / immunology
- Horse Diseases / chemically induced
- Horse Diseases / parasitology
- Horse Diseases / prevention & control
- Horses
- Inflammation / blood
- Inflammation / metabolism
- Larva / drug effects
- Macrolides / adverse effects
- Macrolides / therapeutic use
- Organ Size
- Strongyle Infections, Equine / drug therapy
- Strongyle Infections, Equine / parasitology
- Strongyloidea / drug effects
Citations
This article has been cited 2 times.- Long A, Nolen-Walston R. Equine Inflammatory Markers in the Twenty-First Century: A Focus on Serum Amyloid A. Vet Clin North Am Equine Pract 2020 Apr;36(1):147-160.
- Linardi RL, Dodson ME, Moss KL, King WJ, Ortved KF. The Effect of Autologous Protein Solution on the Inflammatory Cascade in Stimulated Equine Chondrocytes. Front Vet Sci 2019;6:64.
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