Hematologic and immunophenotypic factors associated with development of Rhodococcus equi pneumonia of foals at equine breeding farms with endemic infection.
Abstract: Rhodococcus equi causes severe pyogranulomatous pneumonia in foals and in immunocompromised people. In mice, both CD4+ and CD8+ T lymphocytes contribute to host defense against R. equi, but CD4+ T lymphocytes are required for pulmonary clearance of the bacteria. In this prospective study of 208 foals at two equine breeding farms with endemic R. equi infections, we collected peripheral blood samples at 2 and 4 weeks of age and at the time of diagnosis of R. equi pneumonia. Samples were analyzed for concentrations of total and differential leukocytes, EqCD4+ and EqCD8+ T lymphocytes, and B lymphocytes. Thirty (14.4%) foals developed R. equi pneumonia. At the 2nd week of life, affected foals had significantly lower concentrations of white blood cells (WBC) and segmented neutrophils, significantly lower proportions of EqCD4+ T lymphocytes, and significantly higher proportions of EqCD8+ T lymphocytes. The EqCD4:EqCD8 ratio was significantly lower for affected foals. At the 4th week of life, affected foals had significantly lower concentrations of segmented neutrophils and EqCD4+ T lymphocytes than did unaffected foals. The ratio of EqCD4:EqCD8 was significantly lower for affected foals. Two- and 4-week-old foals with ratios of EqCD4:EqCD8<3 were significantly more likely to develop R. equi pneumonia. There was a significant farm effect which diluted our statistical power to detect differences; however; after adjusting for the farm effect, 2-week-old foals with ratios of EqCD4:EqCD8<3 remained significantly more likely to develop R. equi pneumonia. There were no significant differences in immunophenotypic variables between affected foals (at the time of diagnosis) and age-matched control foals. These data suggest that there are hematologic and immunophenotypic differences between affected and unaffected foals during the first 2-4 weeks of life, prior to onset of clinical signs of R. equi pneumonia. These differences may represent important immunologic mechanisms associated with increased susceptibility of individual foals to infection with R. equi. Because there was considerable overlap between values for affected and unaffected foals, we cannot yet recommend immunophenotyping of foals at endemically-infected farms as a clinically useful screening tool to identify foals at increased risk of developing R. equi pneumonia.
Publication Date: 2004-06-09 PubMed ID: 15182994DOI: 10.1016/j.vetimm.2004.02.010Google Scholar: Lookup
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- Journal Article
- Research Support
- Non-U.S. Gov't
- Research Support
- U.S. Gov't
- Non-P.H.S.
Summary
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This research investigates the association of certain blood and immune responses in foals with the development of Rhodococcus equi pneumonia, a severe infection that frequently affects young horses. The researchers identified significant differences in the immune response of foals that developed the infection compared to those who did not, offering potential insights into the mechanisms of susceptibility.
Insights into the methodology and participant selection
- The study involved a prospective study of 208 foals, from two equine breeding farms with endemic, or constantly present, R. equi infections.
- Peripheral blood samples were taken from the subjects when they were 2 and 4 weeks of age and at the time of diagnosis for R. equi pneumonia.
- Researchers analyzed these samples for concentrations of total and different types of leukocytes, such as T lymphocytes and B lymphocytes.
Differences identified in affected foals
- Of the total sample, 30 foals (14.4%) developed R. equi pneumonia.
- It was found that at 2 weeks old, foals that developed infection had significantly lower concentrations of white blood cells and segmented neutrophils, lower proportions of a particular type of T lymphocyte (EqCD4+), and higher proportions of another type of T lymphocyte (EqCD8+).
- By the 4th week of life, foals with the infection presented lower concentrations of neutrophils and EqCD4+ lymphocytes compared with non-affected foals.
- The study found a significant farm effect that diluted statistical power to detect differences; however, even after adjusting for this effect, the 2-week-old foals with ratios of EqCD4:EqCD8 lower than 3 were found to be significantly more at risk of developing the infection.
Implications and conclusions
- These findings suggest that there are hematologic (relating to blood) and immunophenotypic (relating to the properties of immune cells) differences between affected and unaffected foals, observable within the first 2-4 weeks of life, prior to the onset of clinical signs.
- These differences might indicate significant immune mechanisms associated with an increased susceptibility to infection with R. equi. However, due to the substantial overlap between values for affected and unaffected foals, the researchers caution against using this immunophenotyping as a reliable clinical tool for screening foals at risk of developing R. equi pneumonia.
Cite This Article
APA
Chaffin MK, Cohen ND, Martens RJ, Edwards RF, Nevill M, Smith R.
(2004).
Hematologic and immunophenotypic factors associated with development of Rhodococcus equi pneumonia of foals at equine breeding farms with endemic infection.
Vet Immunol Immunopathol, 100(1-2), 33-48.
https://doi.org/10.1016/j.vetimm.2004.02.010 Publication
Researcher Affiliations
- Department of Large Animal Medicine and Surgery, College of Veterinary Medicine, Texas A&M University, College Station, TX 77843-4475, USA. kchaffin@cvm.tamu.edu
MeSH Terms
- Actinomycetales Infections / immunology
- Actinomycetales Infections / microbiology
- Actinomycetales Infections / veterinary
- Animals
- B-Lymphocytes / immunology
- CD4-CD8 Ratio / veterinary
- CD4-Positive T-Lymphocytes / immunology
- CD8-Positive T-Lymphocytes / immunology
- Flow Cytometry / veterinary
- Horse Diseases / immunology
- Horse Diseases / microbiology
- Horses
- Immunophenotyping / veterinary
- Leukocyte Count / veterinary
- Logistic Models
- Multivariate Analysis
- Neutrophils / immunology
- Pneumonia, Bacterial / immunology
- Pneumonia, Bacterial / microbiology
- Pneumonia, Bacterial / veterinary
- Prospective Studies
- Rhodococcus equi / immunology
Citations
This article has been cited 8 times.- Villalba-Orero M, Gómez CA, Valero-Gónzalez M, Venegas N, Criado G, Martín-Cuervo M. Blood parameters in neonatal foal and colostrum quality as possible early markers for increased risk of developing Rhodococcus equi pneumonia. Front Vet Sci 2025;12:1654052.
- da Silveira BP, Kahn SK, Legere RM, Bray JM, Cole-Pfeiffer HM, Golding MC, Cohen ND, Bordin AI. Enteral immunization with live bacteria reprograms innate immune cells and protects neonatal foals from pneumonia. Sci Rep 2025 May 25;15(1):18156.
- da Silveira BP, Cohen ND, Lawhon SD, Watson RO, Bordin AI. Protective immune response against Rhodococcus equi: An innate immunity-focused review. Equine Vet J 2025 May;57(3):563-586.
- Alvarez Narvaez S, Sanchez S. Exploring the Accessory Genome of Multidrug-Resistant Rhodococcus equi Clone 2287. Antibiotics (Basel) 2023 Nov 17;12(11).
- Cohen ND, Kahn SK, Cywes-Bentley C, Ramirez-Cortez S, Schuckert AE, Vinacur M, Bordin AI, Pier GB. Serum Antibody Activity against Poly-N-Acetyl Glucosamine (PNAG), but Not PNAG Vaccination Status, Is Associated with Protecting Newborn Foals against Intrabronchial Infection with Rhodococcus equi. Microbiol Spectr 2021 Sep 3;9(1):e0063821.
- Cohen ND, Bourquin JR, Bordin AI, Kuskie KR, Brake CN, Weaver KB, Liu M, Felippe MJ, Kogut MH. Intramuscular administration of a synthetic CpG-oligodeoxynucleotide modulates functional responses of neutrophils of neonatal foals. PLoS One 2014;9(10):e109865.
- McQueen CM, Doan R, Dindot SV, Bourquin JR, Zlatev ZZ, Chaffin MK, Blodgett GP, Ivanov I, Cohen ND. Identification of genomic loci associated with Rhodococcus equi susceptibility in foals. PLoS One 2014;9(6):e98710.
- Martens RJ, Cohen ND, Jones SL, Moore TA, Edwards JF. Protective role of neutrophils in mice experimentally infected with Rhodococcus equi. Infect Immun 2005 Oct;73(10):7040-2.
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