Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays

Clinical DNA is often available in limited quantities requiring whole-genome amplification for subsequent genome-wide assessment of copy-number variation (CNV) by array-CGH. In pre-implantation diagnosis and analysis of micrometastases, even merely single cells are available for analysis. However, p...

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Autores principales: Geigl, Jochen B., Obenauf, Anna C., Waldispuehl-Geigl, Julie, Hoffmann, Eva M., Auer, Martina, Hörmann, Martina, Fischer, Maria, Trajanoski, Zlatko, Schenk, Michael A., Baumbusch, Lars O., Speicher, Michael R.
Formato: Texto
Lenguaje:English
Publicado: Oxford University Press 2009
Materias:
Methods Online
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2731907/
https://www.ncbi.nlm.nih.gov/pubmed/19541849
http://dx.doi.org/10.1093/nar/gkp526
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author Geigl, Jochen B.
Obenauf, Anna C.
Waldispuehl-Geigl, Julie
Hoffmann, Eva M.
Auer, Martina
Hörmann, Martina
Fischer, Maria
Trajanoski, Zlatko
Schenk, Michael A.
Baumbusch, Lars O.
Speicher, Michael R.
author_facet Geigl, Jochen B.
Obenauf, Anna C.
Waldispuehl-Geigl, Julie
Hoffmann, Eva M.
Auer, Martina
Hörmann, Martina
Fischer, Maria
Trajanoski, Zlatko
Schenk, Michael A.
Baumbusch, Lars O.
Speicher, Michael R.
author_sort Geigl, Jochen B.
collection PubMed
description Clinical DNA is often available in limited quantities requiring whole-genome amplification for subsequent genome-wide assessment of copy-number variation (CNV) by array-CGH. In pre-implantation diagnosis and analysis of micrometastases, even merely single cells are available for analysis. However, procedures allowing high-resolution analyses of CNVs from single cells well below resolution limits of conventional cytogenetics are lacking. Here, we applied amplification products of single cells and of cell pools (5 or 10 cells) from patients with developmental delay, cancer cell lines and polar bodies to various oligo tiling array platforms with a median probe spacing as high as 65 bp. Our high-resolution analyses reveal that the low amounts of template DNA do not result in a completely unbiased whole genome amplification but that stochastic amplification artifacts, which become more obvious on array platforms with tiling path resolution, cause significant noise. We implemented a new evaluation algorithm specifically for the identification of small gains and losses in such very noisy ratio profiles. Our data suggest that when assessed with sufficiently sensitive methods high-resolution oligo-arrays allow a reliable identification of CNVs as small as 500 kb in cell pools (5 or 10 cells), and of 2.6–3.0 Mb in single cells.
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spelling pubmed-27319072009-09-10 Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays Geigl, Jochen B. Obenauf, Anna C. Waldispuehl-Geigl, Julie Hoffmann, Eva M. Auer, Martina Hörmann, Martina Fischer, Maria Trajanoski, Zlatko Schenk, Michael A. Baumbusch, Lars O. Speicher, Michael R. Nucleic Acids Res Methods Online Clinical DNA is often available in limited quantities requiring whole-genome amplification for subsequent genome-wide assessment of copy-number variation (CNV) by array-CGH. In pre-implantation diagnosis and analysis of micrometastases, even merely single cells are available for analysis. However, procedures allowing high-resolution analyses of CNVs from single cells well below resolution limits of conventional cytogenetics are lacking. Here, we applied amplification products of single cells and of cell pools (5 or 10 cells) from patients with developmental delay, cancer cell lines and polar bodies to various oligo tiling array platforms with a median probe spacing as high as 65 bp. Our high-resolution analyses reveal that the low amounts of template DNA do not result in a completely unbiased whole genome amplification but that stochastic amplification artifacts, which become more obvious on array platforms with tiling path resolution, cause significant noise. We implemented a new evaluation algorithm specifically for the identification of small gains and losses in such very noisy ratio profiles. Our data suggest that when assessed with sufficiently sensitive methods high-resolution oligo-arrays allow a reliable identification of CNVs as small as 500 kb in cell pools (5 or 10 cells), and of 2.6–3.0 Mb in single cells. Oxford University Press 2009-08 2009-06-18 /pmc/articles/PMC2731907/ /pubmed/19541849 http://dx.doi.org/10.1093/nar/gkp526 Text en © 2009 The Author(s) http://creativecommons.org/licenses/by-nc/2.0/uk/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/2.0/uk/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Methods Online
Geigl, Jochen B.
Obenauf, Anna C.
Waldispuehl-Geigl, Julie
Hoffmann, Eva M.
Auer, Martina
Hörmann, Martina
Fischer, Maria
Trajanoski, Zlatko
Schenk, Michael A.
Baumbusch, Lars O.
Speicher, Michael R.
Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title_full Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title_fullStr Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title_full_unstemmed Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title_short Identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
title_sort identification of small gains and losses in single cells after whole genome amplification on tiling oligo arrays
topic Methods Online
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2731907/
https://www.ncbi.nlm.nih.gov/pubmed/19541849
http://dx.doi.org/10.1093/nar/gkp526
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