Compară metode

Examinează metodele selectate una lângă alta; rândurile care diferă sunt evidențiate.

	Analiză Filogenetică la Nivel de Celulă Unică ×	Analiza variației numărului de copii ×
Domeniu	Bioinformatică	Bioinformatică
Familie	Process / pipeline	Process / pipeline
Anul apariției≠	2014-2020 (rapid development period)	1998–2006
Autorul original≠	Multiple groups; foundational tools: Trapnell et al. (Monocle, 2014), Jones et al. (Cassiopeia, 2020)	Pinkel et al. (array CGH); Redon et al. (genome-wide CNV map)
Tip≠	Computational phylogenetic inference pipeline	Genomic structural variant detection pipeline
Sursa seminală≠	Jones, M. G., Khodaverdian, A., Quinn, J. J., Chan, M. M., Hussmann, J. A., Wang, R., Xu, C., Weissman, J. S., & Yosef, N. (2020). Inference of single-cell phylogenies from lineage tracing data using Cassiopeia. Genome Biology, 21(1), 92. DOI ↗	Redon, R., Ishikawa, S., Fitch, K. R., et al. (2006). Global variation in copy number in the human genome. Nature, 444(7118), 444–454. DOI ↗
Denumiri alternative	scPhylogeny, single-cell lineage tracing, clonal phylogenetics, single-cell tree inference	CNV analysis, copy number variant detection, CNV calling, somatic copy number alteration analysis
Înrudite≠	4	6
Rezumat≠	Single-cell phylogenetic analysis reconstructs evolutionary or developmental trees from single-cell sequencing data, tracing how individual cells diverged from a common ancestor. By leveraging somatic mutations, CRISPR-introduced barcodes, or copy-number changes as heritable characters, this method maps clonal relationships within tumors, developing tissues, or immune repertoires with unprecedented cellular resolution.	Copy number variation (CNV) analysis is a genomic pipeline for detecting regions where individuals carry fewer or more copies of a DNA segment than the reference genome. CNVs span kilobases to megabases and are a major class of structural variation implicated in cancer, neurodevelopmental disorders, and population diversity. The pipeline typically processes SNP array intensities or read-depth signals from whole-genome sequencing, applies segmentation algorithms, calls gain and loss events, and annotates them against gene and clinical databases.
ScholarGateSet de date ↗	v1 2 Surse PUBLISHED	v1 2 Surse PUBLISHED

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