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Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform

Although NGS technologies fuel advances in high-throughput HLA genotyping methods for identification and classification of HLA genes to assist with precision medicine efforts in disease and transplantation, the efficiency of these methods are impeded by the absence of adequately-characterized high-f...

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Autores principales: Suzuki, Shingo, Ranade, Swati, Osaki, Ken, Ito, Sayaka, Shigenari, Atsuko, Ohnuki, Yuko, Oka, Akira, Masuya, Anri, Harting, John, Baybayan, Primo, Kitazume, Miwako, Sunaga, Junichi, Morishima, Satoko, Morishima, Yasuo, Inoko, Hidetoshi, Kulski, Jerzy K., Shiina, Takashi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6180199/
https://www.ncbi.nlm.nih.gov/pubmed/30337930
http://dx.doi.org/10.3389/fimmu.2018.02294
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author Suzuki, Shingo
Ranade, Swati
Osaki, Ken
Ito, Sayaka
Shigenari, Atsuko
Ohnuki, Yuko
Oka, Akira
Masuya, Anri
Harting, John
Baybayan, Primo
Kitazume, Miwako
Sunaga, Junichi
Morishima, Satoko
Morishima, Yasuo
Inoko, Hidetoshi
Kulski, Jerzy K.
Shiina, Takashi
author_facet Suzuki, Shingo
Ranade, Swati
Osaki, Ken
Ito, Sayaka
Shigenari, Atsuko
Ohnuki, Yuko
Oka, Akira
Masuya, Anri
Harting, John
Baybayan, Primo
Kitazume, Miwako
Sunaga, Junichi
Morishima, Satoko
Morishima, Yasuo
Inoko, Hidetoshi
Kulski, Jerzy K.
Shiina, Takashi
author_sort Suzuki, Shingo
collection PubMed
description Although NGS technologies fuel advances in high-throughput HLA genotyping methods for identification and classification of HLA genes to assist with precision medicine efforts in disease and transplantation, the efficiency of these methods are impeded by the absence of adequately-characterized high-frequency HLA allele reference sequence databases for the highly polymorphic HLA gene system. Here, we report on producing a comprehensive collection of full-length HLA allele sequences for eight classical HLA loci found in the Japanese population. We augmented the second-generation short read data generated by the Ion Torrent technology with long amplicon spanning consensus reads delivered by the third-generation SMRT sequencing method to create reference grade high-quality sequences of HLA class I and II gene alleles resolved at the genomic coding and non-coding level. Forty-six DNAs were obtained from a reference set used previously to establish the HLA allele frequency data in Japanese subjects. The samples included alleles with a collective allele frequency in the Japanese population of more than 99.2%. The HLA loci were independently amplified by long-range PCR using previously designed HLA-locus specific primers and subsequently sequenced using SMRT and Ion PGM sequencers. The mapped long and short-reads were used to produce a reference library of consensus HLA allelic sequences with the help of the reference-aware software tool LAA for SMRT Sequencing. A total of 253 distinct alleles were determined for 46 healthy subjects. Of them, 137 were novel alleles: 101 SNVs and/or indels and 36 extended alleles at a partial or full-length level. Comparing the HLA sequences from the perspective of nucleotide diversity revealed that HLA-DRB1 was the most divergent among the eight HLA genes, and that the HLA-DPB1 gene sequences diverged into two distinct groups, DP2 and DP5, with evidence of independent polymorphisms generated in exon 2. We also identified two specific intronic variations in HLA-DRB1 that might be involved in rheumatoid arthritis. In conclusion, full-length HLA allele sequencing by third-generation and second-generation technologies has provided polymorphic gene reference sequences at a genomic allelic resolution including allelic variations assigned up to the field-4 level for a stronger foundation in precision medicine and HLA-related disease and transplantation studies.
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spelling pubmed-61801992018-10-18 Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform Suzuki, Shingo Ranade, Swati Osaki, Ken Ito, Sayaka Shigenari, Atsuko Ohnuki, Yuko Oka, Akira Masuya, Anri Harting, John Baybayan, Primo Kitazume, Miwako Sunaga, Junichi Morishima, Satoko Morishima, Yasuo Inoko, Hidetoshi Kulski, Jerzy K. Shiina, Takashi Front Immunol Immunology Although NGS technologies fuel advances in high-throughput HLA genotyping methods for identification and classification of HLA genes to assist with precision medicine efforts in disease and transplantation, the efficiency of these methods are impeded by the absence of adequately-characterized high-frequency HLA allele reference sequence databases for the highly polymorphic HLA gene system. Here, we report on producing a comprehensive collection of full-length HLA allele sequences for eight classical HLA loci found in the Japanese population. We augmented the second-generation short read data generated by the Ion Torrent technology with long amplicon spanning consensus reads delivered by the third-generation SMRT sequencing method to create reference grade high-quality sequences of HLA class I and II gene alleles resolved at the genomic coding and non-coding level. Forty-six DNAs were obtained from a reference set used previously to establish the HLA allele frequency data in Japanese subjects. The samples included alleles with a collective allele frequency in the Japanese population of more than 99.2%. The HLA loci were independently amplified by long-range PCR using previously designed HLA-locus specific primers and subsequently sequenced using SMRT and Ion PGM sequencers. The mapped long and short-reads were used to produce a reference library of consensus HLA allelic sequences with the help of the reference-aware software tool LAA for SMRT Sequencing. A total of 253 distinct alleles were determined for 46 healthy subjects. Of them, 137 were novel alleles: 101 SNVs and/or indels and 36 extended alleles at a partial or full-length level. Comparing the HLA sequences from the perspective of nucleotide diversity revealed that HLA-DRB1 was the most divergent among the eight HLA genes, and that the HLA-DPB1 gene sequences diverged into two distinct groups, DP2 and DP5, with evidence of independent polymorphisms generated in exon 2. We also identified two specific intronic variations in HLA-DRB1 that might be involved in rheumatoid arthritis. In conclusion, full-length HLA allele sequencing by third-generation and second-generation technologies has provided polymorphic gene reference sequences at a genomic allelic resolution including allelic variations assigned up to the field-4 level for a stronger foundation in precision medicine and HLA-related disease and transplantation studies. Frontiers Media S.A. 2018-10-04 /pmc/articles/PMC6180199/ /pubmed/30337930 http://dx.doi.org/10.3389/fimmu.2018.02294 Text en Copyright © 2018 Suzuki, Ranade, Osaki, Ito, Shigenari, Ohnuki, Oka, Masuya, Harting, Baybayan, Kitazume, Sunaga, Morishima, Morishima, Inoko, Kulski and Shiina. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Suzuki, Shingo
Ranade, Swati
Osaki, Ken
Ito, Sayaka
Shigenari, Atsuko
Ohnuki, Yuko
Oka, Akira
Masuya, Anri
Harting, John
Baybayan, Primo
Kitazume, Miwako
Sunaga, Junichi
Morishima, Satoko
Morishima, Yasuo
Inoko, Hidetoshi
Kulski, Jerzy K.
Shiina, Takashi
Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title_full Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title_fullStr Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title_full_unstemmed Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title_short Reference Grade Characterization of Polymorphisms in Full-Length HLA Class I and II Genes With Short-Read Sequencing on the ION PGM System and Long-Reads Generated by Single Molecule, Real-Time Sequencing on the PacBio Platform
title_sort reference grade characterization of polymorphisms in full-length hla class i and ii genes with short-read sequencing on the ion pgm system and long-reads generated by single molecule, real-time sequencing on the pacbio platform
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6180199/
https://www.ncbi.nlm.nih.gov/pubmed/30337930
http://dx.doi.org/10.3389/fimmu.2018.02294
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