Single-cell spatial reconstruction reveals global division of labour in the mammalian liver

single cell sequencing;SNS;单细胞测序;单细胞多组学
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Keren Bahar Halpern #, Rom Shenhav #, Orit Matcovitch-Natan, Beata Toth, Doron Lemze, Matan Golan, Efi E Massasa, Shaked Baydatch, Shanie Landen, Andreas E Moor, Alexander Brandis, Amir Giladi, Avigail Stokar Avihail, Eyal David, Ido Amit, Shalev Itzkovitz

  • Nature
  • 2017
  • 48.5
  • 542(7641):352-356.
  • Mouse
  • 单细胞测序
  • 技术分享
  • Hepatocyte
  • 技术分享
  • 其它细胞
  • ACLY, ALBU, APOA1, ARLY, ASSY, CP2E1, CP2F2, G6PC, GLNA, MUP3, PCKGC
  • doi: 10.1038/nature21065.
  • UBERON_0002107

Abstract

The mammalian liver consists of hexagon-shaped lobules that are radially polarized by blood flow and morphogens. Key liver genes have been shown to be differentially expressed along the lobule axis, a phenomenon termed zonation, but a detailed genome-wide reconstruction of this spatial division of labour has not been achieved. Here we measure the entire transcriptome of thousands of mouse liver cells and infer their lobule coordinates on the basis of a panel of zonated landmark genes, characterized with single-molecule fluorescence in situ hybridization. Using this approach, we obtain the zonation profiles of all liver genes with high spatial resolution. We find that around 50% of liver genes are significantly zonated and uncover abundant non-monotonic profiles that peak at the mid-lobule layers. These include a spatial order of bile acid biosynthesis enzymes that matches their position in the enzymatic cascade. Our approach can facilitate the reconstruction of similar spatial genomic blueprints for other mammalian organs.
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