Non-expression of HLA-A*2901102 N is caused by a nucleotide exchange in the mRNA splicing site at the beginning of intron 4

We describe the identification of the novel human leukocyte antigen (HLA) blank allele A*2901102N which was detected in an individual of mixed race. The serological HLA class I typing was A1; B7,44 whereas PCR-SSP indicated the presence of an additional A*29 allele. The pedigree analysis demonstrated that the new blank allele segregated with the haplotype A*29null B*07, inherited from the individual's Vietnamese father. A single G-->T transversion was detected at position 1 of intron 4, which is a highly conserved nucleotide position in vertebrate splice donor sites. Accordingly it, is very likely that this nucleotide exchange inhibits the splicing of intron 4, is resulting in a premature stop codon further downstream. Despite this alteration, transcription into mRNA was demonstrated.