| Literature DB >> 30107213 |
Christina E M Voorter1, Ben Matern2, Thuong Hien Tran3, Annette Fink3, Blanka Vidan-Jeras4, Sendi Montanic4, Gottfried Fischer5, Ingrid Fae5, Dianne de Santis6, Rebecca Whidborne6, Marco Andreani7, Manuela Testi7, Mathijs Groeneweg2, Marcel G J Tilanus2.
Abstract
The gold standard for typing at the allele level of the highly polymorphic Human Leucocyte Antigen (HLA) gene system is sequence based typing. Since sequencing strategies have mainly focused on identification of the peptide binding groove, full-length sequence information is lacking for >90% of the HLA alleles. One of the goals of the 17th IHIWS workshop is to establish full-length sequences for as many HLA alleles as possible. In our component "Extension of HLA sequences by full-length HLA allele-specific hemizygous Sanger sequencing" we have used full-length hemizygous Sanger Sequence Based Typing to achieve this goal. We selected samples of which full length sequences were not available in the IPD-IMGT/HLA database. In total we have generated the full-length sequences of 48 HLA-A, 45 -B and 31 -C alleles. For HLA-A extended alleles, 39/48 showed no intron differences compared to the first allele of the corresponding allele group, for HLA-B this was 26/45 and for HLA-C 20/31. Comparing the intron sequences to other alleles of the same allele group revealed that in 5/48 HLA-A, 16/45 HLA-B and 8/31 HLA-C alleles the intron sequence was identical to another allele of the same allele group. In the remaining 10 cases, the sequence either showed polymorphism at a conserved nucleotide or was the result of a gene conversion event. Elucidation of the full-length sequence gives insight in the polymorphic content of the alleles and facilitates the identification of its evolutionary origin.Entities:
Keywords: Allele-specific; Full length sequences; HLA alleles; Hemizygous; Sanger Sequence Based Typing
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Year: 2018 PMID: 30107213 DOI: 10.1016/j.humimm.2018.08.004
Source DB: PubMed Journal: Hum Immunol ISSN: 0198-8859 Impact factor: 2.850