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Abstract
Platelet alloimmunization may result in post-transfusion purpura, and during pregnancy
may cause neonatal alloimmune thrombocytopenia (NAIT), with a frequency estimated
at 1.3 per 1000 live births. The risk of morbidity is significant: 20% of affected
infants have neurologic sequelae and the death rate is about 10%. A better understanding
of the immune response to platelet alloantigens would allow for a better definition,
and thus better management of pregnant women at high risk. Limited data are available
on the immune response against HPA-5b, the second most frequent antigen, after HPA-1a,
implicated in NAIT. We studied HLA class II and TAP gene polymorphism in 50 women
immunized against HPA-5 system antigens. Our results suggest a strong association
of alloimmunization with a cluster of HLA DR molecules sharing a particular polymorphic
amino acid sequence at position 69-70 (Glu-Asp encoded by GAA-GAC nucleotide sequence)
of the DR beta 1 chain (RR = 2.95, RR = 5.70 when patients were homozygous for this
sequence), and a negative association with the DRB1*0301 allele (2.1% vs. 28%; RR
= 0.08). Furthermore, increased frequency of a TAP2 dimorphism at position 379 was
observed in immunized women against the HPA-5 antigens (RR = 4.7).