AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome

BACKGROUND: To complement next-generation sequencing technologies, there is a pressing need for efficient pre-sequencing capture methods with reduced costs and DNA requirement. The Alu family of short interspersed nucleotide elements is the most abundant type of transposable elements in the human ge...

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Autores principales: Mei, Lingling, Ding, Xiaofan, Tsang, Shui-Ying, Pun, Frank W, Ng, Siu-Kin, Yang, Jianfeng, Zhao, Cunyou, Li, Dezhi, Wan, Weiqing, Yu, Chi-Hung, Tan, Tze-Ching, Poon, Wai-Sang, Leung, Gilberto Ka-Kit, Ng, Ho-Keung, Zhang, Liwei, Xue, Hong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Methodology Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3228862/
https://www.ncbi.nlm.nih.gov/pubmed/22087792
http://dx.doi.org/10.1186/1471-2164-12-564
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author Mei, Lingling
Ding, Xiaofan
Tsang, Shui-Ying
Pun, Frank W
Ng, Siu-Kin
Yang, Jianfeng
Zhao, Cunyou
Li, Dezhi
Wan, Weiqing
Yu, Chi-Hung
Tan, Tze-Ching
Poon, Wai-Sang
Leung, Gilberto Ka-Kit
Ng, Ho-Keung
Zhang, Liwei
Xue, Hong
author_facet Mei, Lingling
Ding, Xiaofan
Tsang, Shui-Ying
Pun, Frank W
Ng, Siu-Kin
Yang, Jianfeng
Zhao, Cunyou
Li, Dezhi
Wan, Weiqing
Yu, Chi-Hung
Tan, Tze-Ching
Poon, Wai-Sang
Leung, Gilberto Ka-Kit
Ng, Ho-Keung
Zhang, Liwei
Xue, Hong
author_sort Mei, Lingling
collection PubMed
description BACKGROUND: To complement next-generation sequencing technologies, there is a pressing need for efficient pre-sequencing capture methods with reduced costs and DNA requirement. The Alu family of short interspersed nucleotide elements is the most abundant type of transposable elements in the human genome and a recognized source of genome instability. With over one million Alu elements distributed throughout the genome, they are well positioned to facilitate genome-wide sequence amplification and capture of regions likely to harbor genetic variation hotspots of biological relevance. RESULTS: Here we report on the use of inter-Alu PCR with an enhanced range of amplicons in conjunction with next-generation sequencing to generate an Alu-anchored scan, or 'AluScan', of DNA sequences between Alu transposons, where Alu consensus sequence-based 'H-type' PCR primers that elongate outward from the head of an Alu element are combined with 'T-type' primers elongating from the poly-A containing tail to achieve huge amplicon range. To illustrate the method, glioma DNA was compared with white blood cell control DNA of the same patient by means of AluScan. The over 10 Mb sequences obtained, derived from more than 8,000 genes spread over all the chromosomes, revealed a highly reproducible capture of genomic sequences enriched in genic sequences and cancer candidate gene regions. Requiring only sub-micrograms of sample DNA, the power of AluScan as a discovery tool for genetic variations was demonstrated by the identification of 357 instances of loss of heterozygosity, 341 somatic indels, 274 somatic SNVs, and seven potential somatic SNV hotspots between control and glioma DNA. CONCLUSIONS: AluScan, implemented with just a small number of H-type and T-type inter-Alu PCR primers, provides an effective capture of a diversity of genome-wide sequences for analysis. The method, by enabling an examination of gene-enriched regions containing exons, introns, and intergenic sequences with modest capture and sequencing costs, computation workload and DNA sample requirement is particularly well suited for accelerating the discovery of somatic mutations, as well as analysis of disease-predisposing germline polymorphisms, by making possible the comparative genome-wide scanning of DNA sequences from large human cohorts.
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spelling pubmed-32288622011-12-02 AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome Mei, Lingling Ding, Xiaofan Tsang, Shui-Ying Pun, Frank W Ng, Siu-Kin Yang, Jianfeng Zhao, Cunyou Li, Dezhi Wan, Weiqing Yu, Chi-Hung Tan, Tze-Ching Poon, Wai-Sang Leung, Gilberto Ka-Kit Ng, Ho-Keung Zhang, Liwei Xue, Hong BMC Genomics Methodology Article BACKGROUND: To complement next-generation sequencing technologies, there is a pressing need for efficient pre-sequencing capture methods with reduced costs and DNA requirement. The Alu family of short interspersed nucleotide elements is the most abundant type of transposable elements in the human genome and a recognized source of genome instability. With over one million Alu elements distributed throughout the genome, they are well positioned to facilitate genome-wide sequence amplification and capture of regions likely to harbor genetic variation hotspots of biological relevance. RESULTS: Here we report on the use of inter-Alu PCR with an enhanced range of amplicons in conjunction with next-generation sequencing to generate an Alu-anchored scan, or 'AluScan', of DNA sequences between Alu transposons, where Alu consensus sequence-based 'H-type' PCR primers that elongate outward from the head of an Alu element are combined with 'T-type' primers elongating from the poly-A containing tail to achieve huge amplicon range. To illustrate the method, glioma DNA was compared with white blood cell control DNA of the same patient by means of AluScan. The over 10 Mb sequences obtained, derived from more than 8,000 genes spread over all the chromosomes, revealed a highly reproducible capture of genomic sequences enriched in genic sequences and cancer candidate gene regions. Requiring only sub-micrograms of sample DNA, the power of AluScan as a discovery tool for genetic variations was demonstrated by the identification of 357 instances of loss of heterozygosity, 341 somatic indels, 274 somatic SNVs, and seven potential somatic SNV hotspots between control and glioma DNA. CONCLUSIONS: AluScan, implemented with just a small number of H-type and T-type inter-Alu PCR primers, provides an effective capture of a diversity of genome-wide sequences for analysis. The method, by enabling an examination of gene-enriched regions containing exons, introns, and intergenic sequences with modest capture and sequencing costs, computation workload and DNA sample requirement is particularly well suited for accelerating the discovery of somatic mutations, as well as analysis of disease-predisposing germline polymorphisms, by making possible the comparative genome-wide scanning of DNA sequences from large human cohorts. BioMed Central 2011-11-17 /pmc/articles/PMC3228862/ /pubmed/22087792 http://dx.doi.org/10.1186/1471-2164-12-564 Text en Copyright ©2011 Mei et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Methodology Article
Mei, Lingling
Ding, Xiaofan
Tsang, Shui-Ying
Pun, Frank W
Ng, Siu-Kin
Yang, Jianfeng
Zhao, Cunyou
Li, Dezhi
Wan, Weiqing
Yu, Chi-Hung
Tan, Tze-Ching
Poon, Wai-Sang
Leung, Gilberto Ka-Kit
Ng, Ho-Keung
Zhang, Liwei
Xue, Hong
AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title_full AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title_fullStr AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title_full_unstemmed AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title_short AluScan: a method for genome-wide scanning of sequence and structure variations in the human genome
title_sort aluscan: a method for genome-wide scanning of sequence and structure variations in the human genome
topic Methodology Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3228862/
https://www.ncbi.nlm.nih.gov/pubmed/22087792
http://dx.doi.org/10.1186/1471-2164-12-564
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