SCsnvcna: Integrating SNVs and CNAs on a phylogenetic tree from single-cell DNA sequencing data

Zhang, Liting; Bass, Hank W.; Irianto, Jerome; Romanovitch, Mallory

doi:10.1101/2022.08.26.505465

Cited by 1 publication

(1 citation statement)

References 34 publications

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“…Improved tree search algorithms under minimum evolution, as well as strategies for escaping local optima, such as running replicates using resampled bins (analogous to resampling columns of a sequence alignment during phylogenetic bootstrapping), would therefore improve the accuracy of these methods on large datasets. Finally, some recent approaches have combined CNAs and single-nucleotide variants (SNVs) under a single model (Satas et al 2020, Chen et al 2022, Sollier et al 2023, Zhang et al 2023). SNVs, while more challenging to infer accurately from low-coverage single-cell sequencing data than CNAs (Rozhonova et al 2022), could provide additional information and lead to more accurate tumor cell lineage trees.…”

Section: Discussionmentioning

confidence: 99%

DICE: Fast and Accurate Distance-Based Reconstruction of Single-Cell Copy Number Phylogenies

Weiner,

Bansal

2024

Preprint

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Somatic copy number alterations (sCNAs) are valuable phylogenetic markers for inferring evolutionary relationships among tumor cell subpopulations. Advances in single-cell DNA sequencing technologies are making it possible to obtain such sCNAs datasets at ever-larger scales. However, existing methods for reconstructing phylogenies from sCNAs are often too slow for large datasets. Moreover, the accuracies of many existing methods are highly sensitive to error and other features of the analyzed datasets.In this work, we propose two new distance-based approaches for reconstructing single-cell tumor phylogenies from sCNA data. The new methods,DICE-barandDICE-star, are based on novel, easy-to-compute distance measures and drastically outperform the current state-of-the-art in terms of both accuracy and scalability. Using carefully simulated datasets, we find that DICE-bar and DICE-star significantly improve upon the accuracies of existing methods across a wide range of experimental conditions and error rates while simultaneously being orders of magnitude faster. Our experimental analysis also reveals how noise/error in copy number inference, as expected for real datasets, can drastically impact the accuracies of many existing methods. We apply DICE-star, the most accurate method on error-prone datasets, to two real single-cell breast cancer datasets and find that it helps identify previously unreported rare cell populations.

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