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1. CNAsim: improved simulation of single-cell copy number profiles and DNA-seq data from tumors

   https://doi.org/10.1093/bioinformatics/btad434  

   Weiner, Samson; Bansal, Mukul S.; Kendziorski, ed., Christina (July 2023, Bioinformatics)

   Abstract SummaryCNAsim is a software package for improved simulation of single-cell copy number alteration (CNA) data from tumors. CNAsim can be used to efficiently generate single-cell copy number profiles for thousands of simulated tumor cells under a more realistic error model and a broader range of possible CNA mechanisms compared with existing simulators. The error model implemented in CNAsim accounts for the specific biases of single-cell sequencing that leads to read count fluctuation and poor resolution of CNA detection. For improved realism over existing simulators, CNAsim can (i) generate WGD, whole-chromosomal CNAs, and chromosome-arm CNAs, (ii) simulate subclonal population structure defined by the accumulation of chromosomal CNAs, and (iii) dilute the sampled cell population with both normal diploid cells and pseudo-diploid cells. The software can also generate DNA-seq data for sampled cells. Availability and implementationCNAsim is written in Python and is freely available open-source from https://github.com/samsonweiner/CNAsim. 

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2. CNAViz: An interactive webtool for user-guided segmentation of tumor DNA sequencing data

   https://doi.org/10.1371/journal.pcbi.1010614  

   Lalani, Zubair; Chu, Gillian; Hsu, Silas; Kagawa, Shaw; Xiang, Michael; Zaccaria, Simone; El-Kebir, Mohammed (October 2022, PLOS Computational Biology)

   Przytycka, Teresa M. (Ed.)

   Copy-number aberrations (CNAs) are genetic alterations that amplify or delete the number of copies of large genomic segments. Although they are ubiquitous in cancer and, thus, a critical area of current cancer research, CNA identification from DNA sequencing data is challenging because it requires partitioning of the genome into complex segments with the same copy-number states that may not be contiguous. Existing segmentation algorithms address these challenges either by leveraging the local information among neighboring genomic regions, or by globally grouping genomic regions that are affected by similar CNAs across the entire genome. However, both approaches have limitations: overclustering in the case of local segmentation, or the omission of clusters corresponding to focal CNAs in the case of global segmentation. Importantly, inaccurate segmentation will lead to inaccurate identification of CNAs. For this reason, most pan-cancer research studies rely on manual procedures of quality control and anomaly correction. To improve copy-number segmentation, we introduce CNAV iz , a web-based tool that enables the user to simultaneously perform local and global segmentation, thus overcoming the limitations of each approach. Using simulated data, we demonstrate that by several metrics, CNAV iz allows the user to obtain more accurate segmentation relative to existing local and global segmentation methods. Moreover, we analyze six bulk DNA sequencing samples from three breast cancer patients. By validating with parallel single-cell DNA sequencing data from the same samples, we show that by using CNAV iz , our user was able to obtain more accurate segmentation and improved accuracy in downstream copy-number calling. 

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3. CNRein: an evolution-aware deep reinforcement learning algorithm for single-cell DNA copy number calling

   https://doi.org/10.1186/s13059-025-03553-2  

   Ivanovic, Stefan; El-Kebir, Mohammed (April 2025, Genome Biology)

   Abstract Low-pass single-cell DNA sequencing technologies and algorithmic advancements have enabled haplotype-specific copy number calling on thousands of cells within tumors. However, measurement uncertainty may result in spurious CNAs inconsistent with realistic evolutionary constraints. We introduce evolution-aware copy number calling via deep reinforcement learning (CNRein). Our simulations demonstrate CNRein infers more accurate copy-number profiles and better recapitulates ground truth clonal structure than existing methods. On sequencing data of breast and ovarian cancer, CNRein produces more parsimonious solutions than existing methods while maintaining agreement with single-nucleotide variants. Additionally, CNRein shows consistency on a breast cancer patient sequenced with distinct low-pass technologies. 

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4. NestedBD: Bayesian inference of phylogenetic trees from single-cell copy number profiles under a birth-death model

   https://doi.org/10.1186/s13015-024-00264-4  

   Liu, Yushu; Edrisi, Mohammadamin; Yan, Zhi; Ogilvie, Huw; Nakhleh, Luay (December 2024, Algorithms for Molecular Biology)

   Abstract Copy number aberrations (CNAs) are ubiquitous in many types of cancer. Inferring CNAs from cancer genomic data could help shed light on the initiation, progression, and potential treatment of cancer. While such data have traditionally been available via “bulk sequencing,” the more recently introduced techniques for single-cell DNA sequencing (scDNAseq) provide the type of data that makes CNA inference possible at the single-cell resolution. We introduce a new birth-death evolutionary model of CNAs and a Bayesian method, NestedBD, for the inference of evolutionary trees (topologies and branch lengths with relative mutation rates) from single-cell data. We evaluated NestedBD’s performance using simulated data sets, benchmarking its accuracy against traditional phylogenetic tools as well as state-of-the-art methods. The results show that NestedBD infers more accurate topologies and branch lengths, and that the birth-death model can improve the accuracy of copy number estimation. And when applied to biological data sets, NestedBD infers plausible evolutionary histories of two colorectal cancer samples. NestedBD is available athttps://github.com/Androstane/NestedBD. 

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5. CellMeSH: probabilistic cell-type identification using indexed literature

   https://doi.org/10.1093/bioinformatics/btab834  

   Mao, Shunfu; Zhang, Yue; Seelig, Georg; Kannan, Sreeram (February 2022, Bioinformatics)

   Birol, Inanc (Ed.)

   Abstract MotivationSingle-cell RNA sequencing (scRNA-seq) is widely used for analyzing gene expression in multi-cellular systems and provides unprecedented access to cellular heterogeneity. scRNA-seq experiments aim to identify and quantify all cell types present in a sample. Measured single-cell transcriptomes are grouped by similarity and the resulting clusters are mapped to cell types based on cluster-specific gene expression patterns. While the process of generating clusters has become largely automated, annotation remains a laborious ad hoc effort that requires expert biological knowledge. ResultsHere, we introduce CellMeSH—a new automated approach to identifying cell types for clusters based on prior literature. CellMeSH combines a database of gene–cell-type associations with a probabilistic method for database querying. The database is constructed by automatically linking gene and cell-type information from millions of publications using existing indexed literature resources. Compared to manually constructed databases, CellMeSH is more comprehensive and is easily updated with new data. The probabilistic query method enables reliable information retrieval even though the gene–cell-type associations extracted from the literature are noisy. CellMeSH is also able to optionally utilize prior knowledge about tissues or cells for further annotation improvement. CellMeSH achieves top-one and top-three accuracies on a number of mouse and human datasets that are consistently better than existing approaches. Availability and implementationWeb server at https://uncurl.cs.washington.edu/db_query and API at https://github.com/shunfumao/cellmesh. Supplementary informationSupplementary data are available at Bioinformatics online. 

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