A new ABCG2 null allele with a 27‐kb deletion including the promoter region causing the Jr(a−) phenotype
Erythrocytes
Base Sequence
Molecular Sequence Data
Mutation, Missense
Blood Donors
3. Good health
Neoplasm Proteins
03 medical and health sciences
Phenotype
0302 clinical medicine
Blood Group Antigens
ATP Binding Cassette Transporter, Subfamily G, Member 2
Humans
ATP-Binding Cassette Transporters
Promoter Regions, Genetic
Gene Deletion
DOI:
10.1111/trf.12969
Publication Date:
2014-12-19T09:00:07Z
AUTHORS (12)
ABSTRACT
BackgroundThe high‐prevalence antigen Jra is carried on the ATP‐binding cassette transporter ABCG2. The ABCG2 gene consists of 16 exons and its translation start codon is located on the second exon. Although the occurrence of the Jr(a−) phenotype is rare, several ABCG2 null alleles have been reported. We report a new ABCG2 null allele having a large deletion in this study.Study Design and MethodsThe Jra status was determined by standard serologic tests and genomic DNA was isolated from whole blood. Exons 1 to 16 and the 5′‐untranslated region of the ABCG2 gene were analyzed by polymerase chain reaction and sequencing. Expression of the ABCG2 protein on red blood cells was examined by immunoblotting.ResultsA Jr(a−) blood donor had a novel allele having a 27‐kb deletion including noncoding Exon 1 and the promoter region of ABCG2, and the donor was apparently homozygous for the allele. In addition, we found three more individuals having heterozygosity for the same allele, with ABCG2*01N.01 having c.376C>T (p.Q126X), but did not find the allele having the 27‐kb deletion in 3000 Jr(a+) individuals. Immunoblotting revealed that the ABCG2 protein was not found to be expressed in the individual with homozygosity for the ABCG2 27‐kb deleted and in two individuals with an ABCG2 27‐kb deleted/ABCG2*01N.01 genotype, which indirectly allows to conclude that the 27‐kb deletion is responsible for a null ABCG2 allele.ConclusionWe first identified an ABCG2 null allele (provisional ISBT allele number ABCG2*01N.23) having a large deletion including the promoter region.
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CITATIONS (12)
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