Genome-wide detection of single-nucleotide and copy-number variations of a single human cell
- PMID: 23258894
- PMCID: PMC3600412
- DOI: 10.1126/science.1229164
Genome-wide detection of single-nucleotide and copy-number variations of a single human cell
Abstract
Kindred cells can have different genomes because of dynamic changes in DNA. Single-cell sequencing is needed to characterize these genomic differences but has been hindered by whole-genome amplification bias, resulting in low genome coverage. Here, we report on a new amplification method-multiple annealing and looping-based amplification cycles (MALBAC)-that offers high uniformity across the genome. Sequencing MALBAC-amplified DNA achieves 93% genome coverage ≥1x for a single human cell at 25x mean sequencing depth. We detected digitized copy-number variations (CNVs) of a single cancer cell. By sequencing three kindred cells, we were able to identify individual single-nucleotide variations (SNVs), with no false positives detected. We directly measured the genome-wide mutation rate of a cancer cell line and found that purine-pyrimidine exchanges occurred unusually frequently among the newly acquired SNVs.
Conflict of interest statement
CZ, SL and XSX are authors on a patent applied for by Harvard University that covers the MALBAC technology
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Comment in
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Single cells go fully genomic.Nat Methods. 2013 Mar;10(3):190-1. doi: 10.1038/nmeth.2391. Nat Methods. 2013. PMID: 23570041 No abstract available.
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