Abstract 4381

Introduction:

Red blood cell (RBCs) transfusion is the mainstay of treatment for sickle cell disease (SCD) patients and indications continue to expand. Differences in geographic origin between blood donors and sickle recipients has been posited as a cause of the high rate of alloantibodies in patients with sickle cell disease (Vichinsky et al. NEJM 1990; 322: 1617–21). Alloimmunization is one of the major limiting factors of obtaining compatible blood for transfusion and exchange transfusion compromising the management of patients with SCD. Mismatch in minor antigen distribution has been attributed as one of the main reasons for significantly high rate of alloantibodies in SCD patients. Here we describe the minor blood group antigen lacking in SCD patients and comparing with frequencies in white and black populations.

Methods:

Patients with diagnoses of SCD, confirmed by standard hemoglobin electrophoresis, who had at least one type and cross match done from 1995 through 2011 were included in this study. All patients are evaluated for K, C, E, S, Fya, Fyb, Jka and Jkb antigens in addition to ABO and RhD system before transfusion. Results were routinely recorded in the electronic database of the Georgia Comprehensive Sickle Cell Program at Grady Health System to improve patient transfusion management. The frequency of antigens was compared to published prevalence of antigens in Whites and African American population.

Results:

A total of 594 patients were identified with SCD who have been tested for antigens during this period, of these, 310 (52%) females and 284 (48%) males. Average age of the patients is 27 (range 3–84). Most common antigen lacking in SCD patients is from Kell blood group K (98%). About 9% of white population is positive for K. Frequency of E+ is 30% in white population and 2% in blacks while 83% of SCD patients lack E antigen. Overall antigen distribution and comparison included in Table 1.

Conclusion:

Mismatch of antigen expression in white population (mainly donors) especially for K, E, C and Fya; may explain why these are common antibodies detected in SCD patients Anti E (42.3%), Anti C (30.2%), Anti K (28.1%) and Anti Fya (18.3%) (Rosse et al, Blood, Vol 76, No 7). Given these antigen frequency differences, efforts should be made to increase blood donation in the African American population and at least limited phenotypic matching continues to be justified.

Table 1
AntigensSystemFrequency of antigens: Whites %Frequency of antigens: Blacks %Antigens lacking in SCD patients in %
Kell 98 
Fya Duffy 66 10 91 
Fyb Duffy 83 23 78 
Fya+/Fyb- Duffy 17 
Fya-/Fyb+ Duffy 34 22 13 
Fya+/Fyb+ Duffy 49 <1 
Fya-/Fyb- Duffy Very rare 68 71 
Rh 29 22 83 
Rh 98 98 11 
Rh 68 27 75 
Rh 80 96 10 
Jkb Kidd 74 49 59 
Jka Kidd 77 92 16 
Jka+b- Kidd 26.3 51.1 51 
Jka-b+ Kidd 23.4 8.1 
Jka+b+ Kidd 50.3 40.8 33 
Jka-b- Kidd rare rare <1 
MNS 55 31 76 
MNS 89 93 14 
AntigensSystemFrequency of antigens: Whites %Frequency of antigens: Blacks %Antigens lacking in SCD patients in %
Kell 98 
Fya Duffy 66 10 91 
Fyb Duffy 83 23 78 
Fya+/Fyb- Duffy 17 
Fya-/Fyb+ Duffy 34 22 13 
Fya+/Fyb+ Duffy 49 <1 
Fya-/Fyb- Duffy Very rare 68 71 
Rh 29 22 83 
Rh 98 98 11 
Rh 68 27 75 
Rh 80 96 10 
Jkb Kidd 74 49 59 
Jka Kidd 77 92 16 
Jka+b- Kidd 26.3 51.1 51 
Jka-b+ Kidd 23.4 8.1 
Jka+b+ Kidd 50.3 40.8 33 
Jka-b- Kidd rare rare <1 
MNS 55 31 76 
MNS 89 93 14 
View Large
Disclosures:

No relevant conflicts of interest to declare.

Topics:
blood group antigens, health disparity, sickle cell anemia, antigens, transfusion, isoantibodies, alloimmunization, antibodies, blood groups, exchange transfusion, whole blood

Author notes

*

Asterisk with author names denotes non-ASH members.

© 2012 by The American Society of Hematology
2012
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