Warm autoimmune hemolytic anemia with anti‐Jka specificity following babesiosis masquerading as a delayed hemolytic transfusion reaction

Author:

Jacobs Jeremy W.1ORCID,Abels Elizabeth1,Binns Thomas C.1ORCID,Tormey Christopher A.1ORCID,Sostin Nataliya1

Affiliation:

1. Department of Laboratory Medicine Yale School of Medicine New Haven Connecticut USA

Abstract

AbstractBackgroundWarm autoimmune hemolytic anemia (WAIHA) is characterized by the development of autoantibodies that react with red blood cells (RBCs) optimally at physiologic temperature, classically resulting in a positive direct antiglobulin test (DAT) for IgG and a panreactive eluate. Babesiosis has been described as a potentiator of WAIHA, and all cases have shown classic blood bank findings. Only rare reports have described autoantibodies, both secondary to babesiosis and overall, with specificity for Kidd antigens.MethodsAntibody detection and identification were performed using IgG‐specific column agglutination technology. Jka antigen phenotyping was assessed using monoclonal reagents and genotypic analysis was performed at an immunohematology reference laboratory. DATs were performed via standard tube methods. The elution was performed using the ELUclear glycine acid red cell elution kit.ResultsWe report a case of WAIHA induced by Babesia microti infection with an autoantibody with Jka specificity, originally believed to be a delayed hemolytic transfusion reaction, given the detection of an RBC antibody in close proximity to numerous RBC transfusions. Determination of autoantibody status with anti‐Jka‐like reactivity was only confirmed after Kidd antigen genotyping predicted expression of the Jka antigen.DiscussionHealthcare providers should be cognizant of the potential for babesiosis‐induced WAIHA, particularly in individuals who continue to hemolyze despite undetectable parasitemia. Furthermore, this case highlights the possibility for warm autoantibodies to demonstrate Kidd antigen specificity. Though Kidd antigen variants are rare, antigen genotyping may be beneficial, particularly in the context of recent RBC transfusions, which typically preclude accurate serological phenotypic assessment.

Publisher

Wiley

Subject

Hematology,Immunology,Immunology and Allergy

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