Jk3 alloantibodies during pregnancy—blood bank management and hemolytic disease of the fetus and newborn risk

BACKGROUND The Kidd‐null phenotype, Jk(a−b−), occurs in individuals who do not express the JK glycoprotein. Jk(a−b−) individuals can make an antibody against the Jk3 antigen, a high‐incidence antigen present in more than 99.9% of most populations. This presents many challenges to the blood bank including identification of the antibody, masking of other antibodies, and how to provide transfusion support given the rarity of Jk3‐negative blood products. Kidd antibodies may cause acute and delayed hemolytic reactions as well as hemolytic disease of the fetus and newborn (HDFN). In this article, we present a series of four practical cases of pregnant women with the anti‐Jk3 alloantibody that demonstrate a range of clinical presentations of Kidd‐related HDFN. STUDY DESIGN AND METHODS We retrospectively reviewed the clinical and blood bank records for four patients and their newborns encountered at institutions in Tennessee, Missouri, Hawaii, and Guam with an anti‐Jk3 identified during pregnancy. RESULTS Two cases showed no significant evidence for HDFN, while two cases were of mild‐to‐moderate severity requiring early delivery due to elevated middle cerebral artery (MCA) flow velocities but requiring only phototherapy for hyperbilirubinemia. No intrauterine or neonatal transfusions were necessary. Anti‐Jk3 alloantibody titers ranged from 2 to 128. CONCLUSION Clinical manifestations of anti‐Jk3 HDFN are generally mild to moderate. Anti‐Jk3 titers were not found to correlate directly with HDFN severity. We suggest a titer of 16 to 32 as a cutoff for implementing enhanced monitoring of fetal MCA flow velocities, as such titers may be indicative of elevated HDFN risk.