A mechanistic basis for amplification differences between samples and between genome regions

Colin D. Veal; Peter J. Freeman; Kevin Jacobs; Owen Lancaster; Stéphane Jamain; Marion Leboyer; Demetrius Albanes; Reshma R. Vaghela; Ivo Gut; Stephen J. Chanock; Anthony J. Brookes

doi:10.1186/1471-2164-13-455

A mechanistic basis for amplification differences between samples and between genome regions

Colin D. Veal, Peter J. Freeman, Kevin Jacobs, Owen Lancaster, Stéphane Jamain, Marion Leboyer, Demetrius Albanes, Reshma R. Vaghela, Ivo Gut, Stephen J. Chanock, Anthony J. Brookes

Research output: Contribution to journal › Article › peer-review

29 Scopus citations

Abstract

Background: For many analytical methods the efficiency of DNA amplification varies across the genome and between samples. The most affected genome regions tend to correlate with high C + G content, however this relationship is complex and does not explain why the direction and magnitude of effects varies considerably between samples.Results: Here, we provide evidence that sequence elements that are particularly high in C + G content can remain annealed even when aggressive melting conditions are applied. In turn, this behavior creates broader 'Thermodynamically Ultra-Fastened' (TUF) regions characterized by incomplete denaturation of the two DNA strands, so reducing amplification efficiency throughout these domains.Conclusions: This model provides a mechanistic explanation for why some genome regions are particularly difficult to amplify and assay in many procedures, and importantly it also explains inter-sample variability of this behavior. That is, DNA samples of varying quality will carry more or fewer nicks and breaks, and hence their intact TUF regions will have different lengths and so be differentially affected by this amplification suppression mechanism - with 'higher' quality DNAs being the most vulnerable. A major practical consequence of this is that inter-region and inter-sample variability can be largely overcome by employing routine fragmentation methods (e.g. sonication or restriction enzyme digestion) prior to sample amplification.

Original language	English (US)
Article number	455
Journal	BMC genomics
Volume	13
Issue number	1
DOIs	https://doi.org/10.1186/1471-2164-13-455
State	Published - Sep 5 2012
Externally published	Yes

Keywords

C + G
DNA amplification
DNA denaturation
Illumina infinium

ASJC Scopus subject areas

Biotechnology
Genetics

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10.1186/1471-2164-13-455

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title = "A mechanistic basis for amplification differences between samples and between genome regions",

abstract = "Background: For many analytical methods the efficiency of DNA amplification varies across the genome and between samples. The most affected genome regions tend to correlate with high C + G content, however this relationship is complex and does not explain why the direction and magnitude of effects varies considerably between samples.Results: Here, we provide evidence that sequence elements that are particularly high in C + G content can remain annealed even when aggressive melting conditions are applied. In turn, this behavior creates broader 'Thermodynamically Ultra-Fastened' (TUF) regions characterized by incomplete denaturation of the two DNA strands, so reducing amplification efficiency throughout these domains.Conclusions: This model provides a mechanistic explanation for why some genome regions are particularly difficult to amplify and assay in many procedures, and importantly it also explains inter-sample variability of this behavior. That is, DNA samples of varying quality will carry more or fewer nicks and breaks, and hence their intact TUF regions will have different lengths and so be differentially affected by this amplification suppression mechanism - with 'higher' quality DNAs being the most vulnerable. A major practical consequence of this is that inter-region and inter-sample variability can be largely overcome by employing routine fragmentation methods (e.g. sonication or restriction enzyme digestion) prior to sample amplification.",

keywords = "C + G, DNA amplification, DNA denaturation, Illumina infinium",

author = "Veal, {Colin D.} and Freeman, {Peter J.} and Kevin Jacobs and Owen Lancaster and St{\'e}phane Jamain and Marion Leboyer and Demetrius Albanes and Vaghela, {Reshma R.} and Ivo Gut and Chanock, {Stephen J.} and Brookes, {Anthony J.}",

note = "Funding Information: This research was supported by Action Medical Research (grants SP4139 and SP4483) and by the European Union{\textquoteright}s Seventh Framework Programme (FP7/ 2007-2013) project READNA (grant agreement HEALTH-F4-2008-201418). We wish to recognize earlier collaborations particularly with Nancy J Cox from the Division of Biological Sciences, University of Chicago and Paul H Dear and Bernard Konfortov of the MRC laboratory of Molecular Biology (University of Cambridge) that contributed to pointing our experiments towards identifying the TUF phenomenon. The authors wish to thank Ed Schwalbe (University of Newcastle) and Nathalie Zahra (University of Leicester) for their technical support.",

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doi = "10.1186/1471-2164-13-455",

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T1 - A mechanistic basis for amplification differences between samples and between genome regions

AU - Veal, Colin D.

AU - Freeman, Peter J.

AU - Jacobs, Kevin

AU - Lancaster, Owen

AU - Jamain, Stéphane

AU - Leboyer, Marion

AU - Albanes, Demetrius

AU - Vaghela, Reshma R.

AU - Gut, Ivo

AU - Chanock, Stephen J.

AU - Brookes, Anthony J.

N1 - Funding Information: This research was supported by Action Medical Research (grants SP4139 and SP4483) and by the European Union’s Seventh Framework Programme (FP7/ 2007-2013) project READNA (grant agreement HEALTH-F4-2008-201418). We wish to recognize earlier collaborations particularly with Nancy J Cox from the Division of Biological Sciences, University of Chicago and Paul H Dear and Bernard Konfortov of the MRC laboratory of Molecular Biology (University of Cambridge) that contributed to pointing our experiments towards identifying the TUF phenomenon. The authors wish to thank Ed Schwalbe (University of Newcastle) and Nathalie Zahra (University of Leicester) for their technical support.

PY - 2012/9/5

Y1 - 2012/9/5

N2 - Background: For many analytical methods the efficiency of DNA amplification varies across the genome and between samples. The most affected genome regions tend to correlate with high C + G content, however this relationship is complex and does not explain why the direction and magnitude of effects varies considerably between samples.Results: Here, we provide evidence that sequence elements that are particularly high in C + G content can remain annealed even when aggressive melting conditions are applied. In turn, this behavior creates broader 'Thermodynamically Ultra-Fastened' (TUF) regions characterized by incomplete denaturation of the two DNA strands, so reducing amplification efficiency throughout these domains.Conclusions: This model provides a mechanistic explanation for why some genome regions are particularly difficult to amplify and assay in many procedures, and importantly it also explains inter-sample variability of this behavior. That is, DNA samples of varying quality will carry more or fewer nicks and breaks, and hence their intact TUF regions will have different lengths and so be differentially affected by this amplification suppression mechanism - with 'higher' quality DNAs being the most vulnerable. A major practical consequence of this is that inter-region and inter-sample variability can be largely overcome by employing routine fragmentation methods (e.g. sonication or restriction enzyme digestion) prior to sample amplification.

AB - Background: For many analytical methods the efficiency of DNA amplification varies across the genome and between samples. The most affected genome regions tend to correlate with high C + G content, however this relationship is complex and does not explain why the direction and magnitude of effects varies considerably between samples.Results: Here, we provide evidence that sequence elements that are particularly high in C + G content can remain annealed even when aggressive melting conditions are applied. In turn, this behavior creates broader 'Thermodynamically Ultra-Fastened' (TUF) regions characterized by incomplete denaturation of the two DNA strands, so reducing amplification efficiency throughout these domains.Conclusions: This model provides a mechanistic explanation for why some genome regions are particularly difficult to amplify and assay in many procedures, and importantly it also explains inter-sample variability of this behavior. That is, DNA samples of varying quality will carry more or fewer nicks and breaks, and hence their intact TUF regions will have different lengths and so be differentially affected by this amplification suppression mechanism - with 'higher' quality DNAs being the most vulnerable. A major practical consequence of this is that inter-region and inter-sample variability can be largely overcome by employing routine fragmentation methods (e.g. sonication or restriction enzyme digestion) prior to sample amplification.

KW - C + G

KW - DNA amplification

KW - DNA denaturation

KW - Illumina infinium

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A mechanistic basis for amplification differences between samples and between genome regions

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Keywords

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