Phenotype prediction by DNA-based typing of clinically significant blood group systems in Jordanian blood donors

Background and Objectives During the past 10 years several DNA-typing methods have been developed to complement routine serological typing for determination of polymorphisms in the ABO , RH , KEL , JK and FY blood group genes. However, the molecular basis of blood groups can differ widely between ethnic groups. The purpose of this study was to evaluate selected DNA-based methods for phenotype prediction in a population not previously investigated. Materials and Methods Blood samples from a random sample of Jordanian blood donors were collected and red cells isolated from these blood samples were phenotyped for common ABO (n = 150) and KEL/FY/JK (n = 90) antigens. RHD-negative and -positive donors were selected for RH typing (n = 120 and 30, respectively). DNA was prepared and blood group genotyping performed according to selected methods in current use. Discordant samples required further investigation by extended serology and DNA sequencing. Results The degree of concordance between phenotype and genotype was high, but some exceptions were noted. Two of 14 A(2)/A(2)B samples lacked all mutations associated with known A(2) alleles of the ABO system. RH typing revealed four samples with the c(cyt (48) ) marker, causing false-positive RHC typing. A single D-negative sample was positive for D -specific exon 10 markers. The RHD pseudogene was not found in the 150 donors tested. Nine samples revealed discrepancies that were associated with unknown silent or weakly expressing Fy (b) -like alleles. Conclusions With the exception of the FY system, we conclude that the molecular background of the clinically important blood group antigens studied here is similar to that reported for Caucasoids.