Prevalence of a Novel Immunogenic Feline Erythrocyte Antigen (FEA 6) and Expression Patterns Between FEAs

Prevalence of a Novel Immunogenic Feline Erythrocyte Antigen (FEA 6) and Expression Patterns Between FEAs

ABSTRACT Background After the identification of five novel feline erythrocyte antigens (FEAs) and evidence establishing FEA 1's immunogenicity, attempts to sensitize a cat to FEA 4 unexpectedly resulted in the production of alloantibodies directed against an unknown antigen, named FEA 6. Object...

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Bibliographic Details
Main Authors: Félix Bajon, Julie Arsenault, Marie Claude Blais
Format: Article
Language:English
Published: Wiley 2025-05-01
Series:Journal of Veterinary Internal Medicine
Subjects:
alloimmunization
blood typing
crossmatch
Mik antigen
naturally occurring alloantibodies
transfusion
Online Access:https://doi.org/10.1111/jvim.70094
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Summary:ABSTRACT Background After the identification of five novel feline erythrocyte antigens (FEAs) and evidence establishing FEA 1's immunogenicity, attempts to sensitize a cat to FEA 4 unexpectedly resulted in the production of alloantibodies directed against an unknown antigen, named FEA 6. Objectives To estimate the prevalence of FEA 6 as a presumably new antigen, identify corresponding naturally occurring alloantibodies (NOAb), and investigate the associations between known FEAs. Animals Two hundread and seven cats. Methods Prospective blood typing for FEAs 1–6 was conducted in Type A cats (n = 193), followed by serial crossmatching in groups of 3–7 cats to detect NOAb and identify their target FEA. Agreement between FEA 6 blood typing and other FEAs was assessed. Associations between FEAs were evaluated to identify expression patterns. Results Among 193 Type A cats, 67% were FEA 6‐positive. Agreement analyses were supportive of FEA 6 being distinct from FEAs 1–5. NOAb were detected in 11 cats (5.7%), none of which were anti‐FEA 6. Only FEA 1‐negative status was significantly associated with the presence of NOAb (OR = 6.6, 95% CI, 1.9–23.1; p < 0.001). Significant associations were observed between the expressions of FEAs 1 and 4 (χ2 = 25.7, p < 0.001), and FEAs 3 and 5 (Fisher's exact test, p < 0.001), respectively. Conclusions and Clinical Importance The immunogenicity and prevalence of the newly discovered FEA 6 raise concerns regarding its clinical relevance and role in posttransfusion sensitization. FEA 1/FEA 4 and FEA 3/FEA 5 pairs might belong to distinct antigenic systems.
ISSN:0891-6640
1939-1676

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