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

Xin Jin; Mingze He; Betsy Ferguson; Yuhuan Meng; Limei Ouyang; Jingjing Ren; Thomas Mailund; Fei Sun; Liangdan Sun; Juan Shen; Min Zhuo; Li Song; Jufang Wang; Fei Ling; Yuqi Zhu; Christina Hvilsom; Hans Redlef Siegismund; Xiaoming Liu; Zhuolin Gong; Fang Ji; Xinzhong Wang; Boqing Liu; Yu Zhang; Jianguo Hou; Jing Wang; Hua Zhao; Yanyi Wang; Xiaodong Fang; Guojie Zhang; Jian Wang; Xuejun Zhang; Mikkel H. Schierup; Hongli Du; Jun Wang; Xiaoning Wang

doi:10.1371/journal.pone.0040637

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

Xin Jin, Mingze He, Betsy Ferguson, Yuhuan Meng, Limei Ouyang, Jingjing Ren, Thomas Mailund, Fei Sun, Liangdan Sun, Juan Shen, Min Zhuo, Li Song, Jufang Wang, Fei Ling, Yuqi Zhu, Christina Hvilsom, Hans Redlef Siegismund, Xiaoming Liu, Zhuolin Gong, Fang JiXinzhong Wang, Boqing Liu, Yu Zhang, Jianguo Hou, Jing Wang, Hua Zhao, Yanyi Wang, Xiaodong Fang, Guojie Zhang, Jian Wang, Xuejun Zhang, Mikkel H. Schierup, Hongli Du, Jun Wang, Xiaoning Wang

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Abstract

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.

Originalsprog	Engelsk
Tidsskrift	P L o S One
Vol/bind	7
Udgave nummer	7
Antal sider	13
ISSN	1932-6203
DOI	https://doi.org/10.1371/journal.pone.0040637
Status	Udgivet - 27 jul. 2012

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10.1371/journal.pone.0040637

An Effort to Use Human-Based Exome Capture Methods to Analyze Chimpanzee and Macaque ExomesForlagets udgivne version, 438 KB

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Jin, X., He, M., Ferguson, B., Meng, Y., Ouyang, L., Ren, J., Mailund, T., Sun, F., Sun, L., Shen, J., Zhuo, M., Song, L., Wang, J., Ling, F., Zhu, Y., Hvilsom, C., Siegismund, H. R., Liu, X., Gong, Z., ... Wang, X. (2012). An effort to use human-based exome capture methods to analyze chimpanzee and macaque exomes. P L o S One, 7(7). https://doi.org/10.1371/journal.pone.0040637

Jin, X, He, M, Ferguson, B, Meng, Y, Ouyang, L, Ren, J, Mailund, T, Sun, F, Sun, L, Shen, J, Zhuo, M, Song, L, Wang, J, Ling, F, Zhu, Y, Hvilsom, C, Siegismund, HR, Liu, X, Gong, Z, Ji, F, Wang, X, Liu, B, Zhang, Y, Hou, J, Wang, J, Zhao, H, Wang, Y, Fang, X, Zhang, G, Wang, J, Zhang, X, Schierup, MH, Du, H, Wang, J & Wang, X 2012, 'An effort to use human-based exome capture methods to analyze chimpanzee and macaque exomes', P L o S One, bind 7, nr. 7. https://doi.org/10.1371/journal.pone.0040637

@article{c85aba88c00240dc870798ce3fbe50bd,

title = "An effort to use human-based exome capture methods to analyze chimpanzee and macaque exomes",

abstract = "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.",

author = "Xin Jin and Mingze He and Betsy Ferguson and Yuhuan Meng and Limei Ouyang and Jingjing Ren and Thomas Mailund and Fei Sun and Liangdan Sun and Juan Shen and Min Zhuo and Li Song and Jufang Wang and Fei Ling and Yuqi Zhu and Christina Hvilsom and Siegismund, {Hans Redlef} and Xiaoming Liu and Zhuolin Gong and Fang Ji and Xinzhong Wang and Boqing Liu and Yu Zhang and Jianguo Hou and Jing Wang and Hua Zhao and Yanyi Wang and Xiaodong Fang and Guojie Zhang and Jian Wang and Xuejun Zhang and Schierup, {Mikkel H.} and Hongli Du and Jun Wang and Xiaoning Wang",

note = "e40637",

year = "2012",

month = jul,

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doi = "10.1371/journal.pone.0040637",

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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 Redlef

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

N1 - e40637

PY - 2012/7/27

Y1 - 2012/7/27

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

JO - PLoS Computational Biology

JF - PLoS Computational Biology

IS - 7

ER -

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

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