1. Silent <italic>KEL</italic> alleles identified from Japanese individuals with the Ko phenotype.
- Author
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Onodera, T., Kawai, M., Obara, K., Enomoto, T., Sasaki, K., Osabe, T., Ogasawara, K., Toyoda, C., Tsuneyama, H., Uchikawa, M., Inaba, S., and Satake, M.
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PHENOTYPES ,KELL blood group system ,ANTIGENS ,MOLECULAR genetics ,BLOOD donors ,POLYMERASE chain reaction - Abstract
Background and Objective: The rare K
o phenotype lacks all 36 antigens in the Kell blood system. The molecular basis of the Ko phenotype has been investigated, and more than 40 silentKEL alleles are reported by many investigators. The majority of silent alleles are theKEL*02 background. Here, we report molecular genetic analysis of theKEL gene in Japanese individuals with the Ko phenotype. Materials and Methods: The Ko phenotype was screened from Japanese blood donors for several years using monoclonal anti‐Ku or anti‐K14 by an automated blood grouping system PK7300. Kell‐related antigens were typed by standard tube tests. Genomic DNA was extracted from the blood samples, andKEL gene was analysed by polymerase chain reaction (PCR) and Sanger sequencing. Results: We collected 35 Ko blood samples with K−k−, Kp(a−b−), Js(a−b−) and K14−. PCR and sequence analysis revealed that 11 individuals were homozygous for a mutantKEL allele with a c.299G>C (p.Cys100Ser) mutation (rs. 200268316). Three individuals were homozygous for theKEL*02N.24 allele that is c.715G>T (p.Glu239*), and one individual was homozygous for theKEL*02N.40 allele that is c.1474C>T (p.Arg492*). Five individuals were homozygous for novelKEL alleles with single‐nucleotide mutations, four individuals had a c.2175delC (p.Pro725 fs*43), and one individual had a c.328delA (p.Arg110 fs*79). The remaining 15 individuals were compound heterozygous, and eight new alleles were identified from them. Conclusions: We identified three known and ten new silentKEL alleles from Japanese individuals with the Ko phenotype. TheKEL allele with the c.299G>C (p.Cys100Ser) mutation was the most frequent. [ABSTRACT FROM AUTHOR]- Published
- 2018
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