Complete next-generation sequencing: establishment of reference alleles.

Blood Adv

Faculty of Medicine and Dentistry, School of Biomedical Sciences, University of Plymouth, Plymouth, United Kingdom; and.

Published: October 2018

The Rh blood group system (ISBT004) is the second most important blood group after ABO and is the most polymorphic one, with 55 antigens encoded by 2 genes, and This research uses next-generation sequencing (NGS) to sequence the complete gene by amplifying the whole gene using overlapping long-range polymerase chain reaction (LR-PCR) amplicons. The aim was to study different alleles present in the population to establish reference allele sequences by using the analysis of intronic single-nucleotide polymorphisms (SNPs) and their correlation to a specific Rh haplotype. Genomic DNA samples (n = 69) from blood donors of different serologically predicted genotypes including RR (DCe/DCe), RR (DcE/DcE), RR (DCe/DcE), RR (DcE/DCE), Rr (DCe/dce), Rr (DcE/dce), and Rr (Dce/dce) were sequenced and data were then mapped to the human genome reference sequence hg38. We focused on the analysis of hemizygous samples, as these by definition will only have a single copy of For the 69 samples sequenced, different exonic SNPs were detected that correlate with known variants. Multiple intronic SNPs were found in all samples: 21 intronic SNPs were present in all samples indicating their specificity to the haplotype which the hg38 reference sequence encodes. Twenty-three intronic SNPs were found to be R haplotype specific, and 15 were linked to R, R, and R haplotypes. In conclusion, intronic SNPs may represent a novel diagnostic approach to investigate known and novel variants of the and genes, while being a useful approach to establish reference allele sequences.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6199663PMC
http://dx.doi.org/10.1182/bloodadvances.2018017871DOI Listing

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