Literature DB >> 28135258

Sequencing thousands of single-cell genomes with combinatorial indexing.

Sarah A Vitak1, Kristof A Torkenczy1,2, Jimi L Rosenkrantz1,2,3, Andrew J Fields1, Lena Christiansen4, Melissa H Wong5,6, Lucia Carbone1,3,7,8, Frank J Steemers4, Andrew Adey1,8.   

Abstract

Single-cell genome sequencing has proven valuable for the detection of somatic variation, particularly in the context of tumor evolution. Current technologies suffer from high library construction costs, which restrict the number of cells that can be assessed and thus impose limitations on the ability to measure heterogeneity within a tissue. Here, we present single-cell combinatorial indexed sequencing (SCI-seq) as a means of simultaneously generating thousands of low-pass single-cell libraries for detection of somatic copy-number variants. We constructed libraries for 16,698 single cells from a combination of cultured cell lines, primate frontal cortex tissue and two human adenocarcinomas, and obtained a detailed assessment of subclonal variation within a pancreatic tumor.

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Mesh:

Year:  2017        PMID: 28135258      PMCID: PMC5908213          DOI: 10.1038/nmeth.4154

Source DB:  PubMed          Journal:  Nat Methods        ISSN: 1548-7091            Impact factor:   28.547


  34 in total

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Authors:  Jimi L Rosenkrantz; Lucia Carbone
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Journal:  Nature       Date:  2014-11-26       Impact factor: 49.962

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8.  Assessment of megabase-scale somatic copy number variation using single-cell sequencing.

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6.  Exponential scaling of single-cell RNA-seq in the past decade.

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7.  Haplotype resolution at the single-cell level.

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Review 8.  Advancing Cancer Research and Medicine with Single-Cell Genomics.

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9.  A Single-Cell Atlas of In Vivo Mammalian Chromatin Accessibility.

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10.  Single-Cell RNA Sequencing of Ovarian Cancer: Promises and Challenges.

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