An effort to use human-based exome capture methods to analyze chimpanzee and macaque exomes

TY - JOUR

T1 - An effort to use human-based exome capture methods to analyze chimpanzee and macaque exomes

AU - Jin, Xin

AU - He, Mingze

AU - Ferguson, Betsy

AU - Meng, Yuhuan

AU - Ouyang, Limei

AU - Ren, Jingjing

AU - Mailund, Thomas

AU - Sun, Fei

AU - Sun, Liangdan

AU - Shen, Juan

AU - Zhuo, Min

AU - Song, Li

AU - Wang, Jufang

AU - Ling, Fei

AU - Zhu, Yuqi

AU - Hvilsom, Christina

AU - Siegismund, Hans

AU - Liu, Xiaoming

AU - Gong, Zhuolin

AU - Ji, Fang

AU - Wang, Xinzhong

AU - Liu, Boqing

AU - Zhang, Yu

AU - Hou, Jianguo

AU - Wang, Jing

AU - Zhao, Hua

AU - Wang, Yanyi

AU - Fang, Xiaodong

AU - Zhang, Guojie

AU - Wang, Jian

AU - Zhang, Xuejun

AU - Schierup, Mikkel H

AU - Du, Hongli

AU - Wang, Jun

AU - Wang, Xiaoning

PY - 2012

Y1 - 2012

N2 - Non-human primates have emerged as an important resource for the study of human disease and evolution. The characterization of genomic variation between and within non-human primate species could advance the development of genetically defined non-human primate disease models. However, non-human primate specific reagents that would expedite such research, such as exon-capture tools, are lacking. We evaluated the efficiency of using a human exome capture design for the selective enrichment of exonic regions of non-human primates. We compared the exon sequence recovery in nine chimpanzees, two crab-eating macaques and eight Japanese macaques. Over 91% of the target regions were captured in the non-human primate samples, although the specificity of the capture decreased as evolutionary divergence from humans increased. Both intra-specific and inter-specific DNA variants were identified; Sanger-based resequencing validated 85.4% of 41 randomly selected SNPs. Among the short indels identified, a majority (54.6%-77.3%) of the variants resulted in a change of 3 base pairs, consistent with expectations for a selection against frame shift mutations. Taken together, these findings indicate that use of a human design exon-capture array can provide efficient enrichment of non-human primate gene regions. Accordingly, use of the human exon-capture methods provides an attractive, cost-effective approach for the comparative analysis of non-human primate genomes, including gene-based DNA variant discovery.

AB - Non-human primates have emerged as an important resource for the study of human disease and evolution. The characterization of genomic variation between and within non-human primate species could advance the development of genetically defined non-human primate disease models. However, non-human primate specific reagents that would expedite such research, such as exon-capture tools, are lacking. We evaluated the efficiency of using a human exome capture design for the selective enrichment of exonic regions of non-human primates. We compared the exon sequence recovery in nine chimpanzees, two crab-eating macaques and eight Japanese macaques. Over 91% of the target regions were captured in the non-human primate samples, although the specificity of the capture decreased as evolutionary divergence from humans increased. Both intra-specific and inter-specific DNA variants were identified; Sanger-based resequencing validated 85.4% of 41 randomly selected SNPs. Among the short indels identified, a majority (54.6%-77.3%) of the variants resulted in a change of 3 base pairs, consistent with expectations for a selection against frame shift mutations. Taken together, these findings indicate that use of a human design exon-capture array can provide efficient enrichment of non-human primate gene regions. Accordingly, use of the human exon-capture methods provides an attractive, cost-effective approach for the comparative analysis of non-human primate genomes, including gene-based DNA variant discovery.

U2 - 10.1371/journal.pone.0040637

DO - 10.1371/journal.pone.0040637

M3 - Journal article

C2 - 22848389

SN - 1932-6203

VL - 7

SP - e40637

JO - PLoS One

JF - PLoS One

IS - 7

ER -