The yield of universal antibody to hepatitis B core antigen donor screening in the N etherlands, a hepatitis B virus low‐endemic country

Background In the N etherlands, universal antibody to hepatitis B core antigen (anti‐ HBc ) donor screening was introduced in J uly 2011 to intercept potentially infectious donations slipping through hepatitis B surface antigen ( HBsAg ) and hepatitis B virus ( HBV ) DNA minipool screening ( HBV DNA MP 6). Study Design and Methods The yield and donor loss were evaluated after the first 2 years of universal anti‐ HBc donor screening. A total of 382,173 donors were tested for anti‐ HBc and, if positive, for antibody to HBsAg (anti‐ HBs ). Anti‐ HBc –reactive donors with anti‐ HBs of less than 200  IU / L were deferred, but repeat donors were allowed retesting after 6 months if anti‐ HBs was less than 10  IU / mL . Anti‐ HBc false positivity was estimated using the crude anti‐ HBc signal, family name–based ethnicity scoring, and donor follow‐up. Results Anti‐ HBc screening identified 13 confirmed or potential HBsAg ‐ and HBV DNA MP 6–negative recent HBV infections. In addition, 820 anti‐ HBc –reactive donors with low anti‐ HBs titers (<200  IU / mL ), potentially harboring occult HBV infection ( OBI ), were identified and deferred. Overall, 1583 (0.41%) donors were deferred: 1178 (0.31%) during first‐time anti‐ HBc screening, 361 (0.09%) anti‐ HBc seroconverters, and 44 (0.01%) donors with waning anti‐ HBs titers. Only 188 of 1583 (12%) deferred donors could be reentered upon retesting. Estimated anti‐ HBc false positivity was 16%, but varied greatly among anti‐ HBc –reactive donors with and without anti‐ HBs (8% vs. 62%). Conclusion Anti‐ HBc testing has improved the safety of the D utch blood supply but its exact yield remains difficult to determine, due to the complexity of confirming anti‐ HBc reactivity and OBI . In a low‐endemic country, donor loss associated with anti‐ HBc screening is sustainable, but adds to the already considerable list of donor exclusions.