Comprehensive Single-cell Genome Analysis at Nucleotide Resolution Using the PTA Analysis Toolbox

Overview

Journal Cell Genom

Date 2023 Sep 18

PMID 37719152

Authors

Sjors Middelkamp

Freek Manders

Flavia Peci

Markus J van Roosmalen

Diego Montiel Gonzalez

Eline J M Bertrums

Inge van der Werf

Lucca L M Derks

Niels M Groenen

Mark Verheul

Laurianne Trabut

Cayetano Pleguezuelos-Manzano

Arianne M Brandsma

Evangelia Antoniou

Dirk Reinhardt

Marc Bierings

Mirjam E Belderbos

Ruben van Boxtel

Affiliations

Soon will be listed here.

Abstract

Detection of somatic mutations in single cells has been severely hampered by technical limitations of whole-genome amplification. Novel technologies including primary template-directed amplification (PTA) significantly improved the accuracy of single-cell whole-genome sequencing (WGS) but still generate hundreds of artifacts per amplification reaction. We developed a comprehensive bioinformatic workflow, called the PTA Analysis Toolbox (PTATO), to accurately detect single base substitutions, insertions-deletions (indels), and structural variants in PTA-based WGS data. PTATO includes a machine learning approach and filtering based on recurrence to distinguish PTA artifacts from true mutations with high sensitivity (up to 90%), outperforming existing bioinformatic approaches. Using PTATO, we demonstrate that hematopoietic stem cells of patients with Fanconi anemia, which cannot be analyzed using regular WGS, have normal somatic single base substitution burdens but increased numbers of deletions. Our results show that PTATO enables studying somatic mutagenesis in the genomes of single cells with unprecedented sensitivity and accuracy.

Citing Articles

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