Long-read sequencing and de novo assembly of a Chinese genome.
Lingling ShiYunfei GuoChengliang DongJohn HuddlestonHui YangXiaolu HanAisi FuQuan LiNa LiSiyi GongKatherine E LintnerQiong DingZou WangJiang HuDepeng WangFeng WangLin WangGholson J LyonYongtao GuanYufeng ShenOleg V EvgrafovJames A KnowlesFrancoise Thibaud-NissenValerie SchneiderChack-Yung YuLibing ZhouEvan E EichlerKwok-Fai SoKai WangPublished in: Nature communications (2016)
Short-read sequencing has enabled the de novo assembly of several individual human genomes, but with inherent limitations in characterizing repeat elements. Here we sequence a Chinese individual HX1 by single-molecule real-time (SMRT) long-read sequencing, construct a physical map by NanoChannel arrays and generate a de novo assembly of 2.93 Gb (contig N50: 8.3 Mb, scaffold N50: 22.0 Mb, including 39.3 Mb N-bases), together with 206 Mb of alternative haplotypes. The assembly fully or partially fills 274 (28.4%) N-gaps in the reference genome GRCh38. Comparison to GRCh38 reveals 12.8 Mb of HX1-specific sequences, including 4.1 Mb that are not present in previously reported Asian genomes. Furthermore, long-read sequencing of the transcriptome reveals novel spliced genes that are not annotated in GENCODE and are missed by short-read RNA-Seq. Our results imply that improved characterization of genome functional variation may require the use of a range of genomic technologies on diverse human populations.