Copy Number and Loss of Heterozygosity Detected by SNP Array of Formalin-Fixed Tissues Using Whole-Genome Amplification

A Dutt; A Siwoski; Affymetrix; Angela Stokes; BS Carvalho; Christos A. Ouzounis; DL Barker; Edward W. Odell; Eliete Guerra; ER Thompson; FB Dean; H Jeong; Hassan Ashktorab; HY Chuang; Ignat Drozdov; J Huang; J Xing; JA Blake; JJ Corneveaux; JM Korn; JW Park; M Tuefferd; Mahvash Tavassoli; Mark McGurk; Michael J. Gleeson; NM Luscombe; P Flicek; PF Jonsson; S Hughes; S Jacobs; S Mead; SA Forbes; Saman Warnakulasuriya; TJ Pugh; VD Blondel

Copy Number and Loss of Heterozygosity Detected by SNP Array of Formalin-Fixed Tissues Using Whole-Genome Amplification

Authors: A Dutt
A Siwoski
Affymetrix
Angela Stokes
BS Carvalho
Christos A. Ouzounis
DL Barker
Edward W. Odell
Eliete Guerra
ER Thompson
FB Dean
H Jeong
Hassan Ashktorab
HY Chuang
Ignat Drozdov
J Huang
J Xing
JA Blake
JJ Corneveaux
JM Korn
JW Park
M Tuefferd
Mahvash Tavassoli
Mark McGurk
Michael J. Gleeson
NM Luscombe
P Flicek
PF Jonsson
S Hughes
S Jacobs
S Mead
SA Forbes
Saman Warnakulasuriya
TJ Pugh
VD Blondel
Publication date: 1 January 2011
Publisher: Public Library of Science
Doi

Abstract

The requirement for large amounts of good quality DNA for whole-genome applications prohibits their use for small, laser capture micro-dissected (LCM), and/or rare clinical samples, which are also often formalin-fixed and paraffin-embedded (FFPE). Whole-genome amplification of DNA from these samples could, potentially, overcome these limitations. However, little is known about the artefacts introduced by amplification of FFPE-derived DNA with regard to genotyping, and subsequent copy number and loss of heterozygosity (LOH) analyses. Using a ligation adaptor amplification method, we present data from a total of 22 Affymetrix SNP 6.0 experiments, using matched paired amplified and non-amplified DNA from 10 LCM FFPE normal and dysplastic oral epithelial tissues, and an internal method control. An average of 76.5% of SNPs were called in both matched amplified and non-amplified DNA samples, and concordance was a promising 82.4%. Paired analysis for copy number, LOH, and both combined, showed that copy number changes were reduced in amplified DNA, but were 99.5% concordant when detected, amplifications were the changes most likely to be ‘missed’, only 30% of non-amplified LOH changes were identified in amplified pairs, and when copy number and LOH are combined ∼50% of gene changes detected in the unamplified DNA were also detected in the amplified DNA and within these changes, 86.5% were concordant for both copy number and LOH status. However, there are also changes introduced as ∼20% of changes in the amplified DNA are not detected in the non-amplified DNA. An integrative network biology approach revealed that changes in amplified DNA of dysplastic oral epithelium localize to topologically critical regions of the human protein-protein interaction network, suggesting their functional implication in the pathobiology of this disease. Taken together, our results support the use of amplification of FFPE-derived DNA, provided sufficient samples are used to increase power and compensate for increased error rates