Author
Listed:
- Jun Takayama
(Tohoku University
Tohoku University
Statistical Genetics Team, RIKEN Center for Advanced Intelligence Project, Nihonbashi 1-chome Mitsui Building 15F)
- Shu Tadaka
(Tohoku University)
- Kenji Yano
(Tohoku University
Statistical Genetics Team, RIKEN Center for Advanced Intelligence Project, Nihonbashi 1-chome Mitsui Building 15F)
- Fumiki Katsuoka
(Tohoku University
Tohoku University)
- Chinatsu Gocho
(Tohoku University)
- Takamitsu Funayama
(Tohoku University)
- Satoshi Makino
(Tohoku University)
- Yasunobu Okamura
(Tohoku University
Tohoku University)
- Atsuo Kikuchi
(Tohoku University Graduate School of Medicine)
- Sachiyo Sugimoto
(Tohoku University)
- Junko Kawashima
(Tohoku University)
- Akihito Otsuki
(Tohoku University)
- Mika Sakurai-Yageta
(Tohoku University)
- Jun Yasuda
(Tohoku University
Miyagi Cancer Center Research Institute)
- Shigeo Kure
(Tohoku University
Tohoku University Graduate School of Medicine)
- Kengo Kinoshita
(Tohoku University
Tohoku University
Tohoku University)
- Masayuki Yamamoto
(Tohoku University
Tohoku University)
- Gen Tamiya
(Tohoku University
Tohoku University
Statistical Genetics Team, RIKEN Center for Advanced Intelligence Project, Nihonbashi 1-chome Mitsui Building 15F
Tohoku University Graduate School of Medicine)
Abstract
The complete human genome sequence is used as a reference for next-generation sequencing analyses. However, some ethnic ancestries are under-represented in the reference genome (e.g., GRCh37) due to its bias toward European and African ancestries. Here, we perform de novo assembly of three Japanese male genomes using > 100× Pacific Biosciences long reads and Bionano Genomics optical maps per sample. We integrate the genomes using the major allele for consensus and anchor the scaffolds using genetic and radiation hybrid maps to reconstruct each chromosome. The resulting genome sequence, JG1, is contiguous, accurate, and carries the Japanese major allele at most loci. We adopt JG1 as the reference for confirmatory exome re-analyses of seven rare-disease Japanese families and find that re-analysis using JG1 reduces total candidate variant calls versus GRCh37 while retaining disease-causing variants. These results suggest that integrating multiple genomes from a single population can aid genome analyses of that population.
Suggested Citation
Jun Takayama & Shu Tadaka & Kenji Yano & Fumiki Katsuoka & Chinatsu Gocho & Takamitsu Funayama & Satoshi Makino & Yasunobu Okamura & Atsuo Kikuchi & Sachiyo Sugimoto & Junko Kawashima & Akihito Otsuki, 2021.
"Construction and integration of three de novo Japanese human genome assemblies toward a population-specific reference,"
Nature Communications, Nature, vol. 12(1), pages 1-14, December.
Handle:
RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-020-20146-8
DOI: 10.1038/s41467-020-20146-8
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