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A direct comparison of interphase FISH versus low-coverage single cell sequencing to detect aneuploidy reveals respective strengths and weaknesses.

Authors :
Andriani, Grasiella A
Andriani, Grasiella A
Maggi, Elaine
Piqué, Daniel
Zimmerman, Samuel E
Lee, Moonsook
Quispe-Tintaya, Wilber
Maslov, Alexander
Campisi, Judith
Vijg, Jan
Mar, Jessica C
Montagna, Cristina
Andriani, Grasiella A
Andriani, Grasiella A
Maggi, Elaine
Piqué, Daniel
Zimmerman, Samuel E
Lee, Moonsook
Quispe-Tintaya, Wilber
Maslov, Alexander
Campisi, Judith
Vijg, Jan
Mar, Jessica C
Montagna, Cristina
Source :
Scientific reports; vol 9, iss 1, 10508; 2045-2322
Publication Year :
2019

Abstract

Aneuploidy has been reported to occur at remarkably high levels in normal somatic tissues using Fluorescence In Situ Hybridization (FISH). Recently, these reports were contradicted by single-cell low-coverage whole genome sequencing (scL-WGS) analyses, which showed aneuploidy frequencies at least an order of magnitude lower. To explain these seemingly contradictory findings, we used both techniques to analyze artificially generated mock aneuploid cells and cells with natural random aneuploidy. Our data indicate that while FISH tended to over-report aneuploidies, a modified 2-probe approach can accurately detect low levels of aneuploidy. Further, scL-WGS tends to underestimate aneuploidy levels, especially in a polyploid background.

Details

Database :
OAIster
Journal :
Scientific reports; vol 9, iss 1, 10508; 2045-2322
Notes :
application/pdf, Scientific reports vol 9, iss 1, 10508 2045-2322
Publication Type :
Electronic Resource
Accession number :
edsoai.on1287435108
Document Type :
Electronic Resource