AI Article Synopsis

  • Mammalian interphase chromosomes have large lamina-associated domains (LADs) that interact with the nuclear lamina (NL), with a core structure of consistent gene-poor LADs and more variable LADs that differ across cell types.
  • A study mapping NL contacts in nearly 400 single human cells shows that these contacts vary with cell type and are affected by changes in genome ploidy, featuring extensive multivalent interactions over long distances.
  • The findings reveal that consistent NL contacts are linked to lower gene activity and correlate with specific histone modifications, emphasizing key aspects of chromatin organization at the single-cell level.

Article Abstract

Mammalian interphase chromosomes interact with the nuclear lamina (NL) through hundreds of large lamina-associated domains (LADs). We report a method to map NL contacts genome-wide in single human cells. Analysis of nearly 400 maps reveals a core architecture consisting of gene-poor LADs that contact the NL with high cell-to-cell consistency, interspersed by LADs with more variable NL interactions. The variable contacts tend to be cell-type specific and are more sensitive to changes in genome ploidy than the consistent contacts. Single-cell maps indicate that NL contacts involve multivalent interactions over hundreds of kilobases. Moreover, we observe extensive intra-chromosomal coordination of NL contacts, even over tens of megabases. Such coordinated loci exhibit preferential interactions as detected by Hi-C. Finally, the consistency of NL contacts is inversely linked to gene activity in single cells and correlates positively with the heterochromatic histone modification H3K9me3. These results highlight fundamental principles of single-cell chromatin organization. VIDEO ABSTRACT.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4583798PMC
http://dx.doi.org/10.1016/j.cell.2015.08.040DOI Listing

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