Folding and organization of a contiguous chromosome region according to the gene distribution pattern in primary genomic sequence

Author:

Shopland Lindsay S.12,Lynch Christopher R.12,Peterson Kevin A.13,Thornton Kathleen3,Kepper Nick4,Hase Johann von24,Stein Stefan4,Vincent Sarah3,Molloy Kelly R.15,Kreth Gregor4,Cremer Christoph124,Bult Carol J.1,O'Brien Timothy P.12

Affiliation:

1. The Jackson Laboratory, Bar Harbor, ME 04609

2. Institute for Molecular Biophysics

3. Program in Functional Genomics, University of Maine, Orono, ME 04469

4. Kirchhoff Institute for Physics, University of Heidelberg, D-69120 Germany

5. Department of Physics, Brown University, Providence, RI 02912

Abstract

Specific mammalian genes functionally and dynamically associate together within the nucleus. Yet, how an array of many genes along the chromosome sequence can be spatially organized and folded together is unknown. We investigated the 3D structure of a well-annotated, highly conserved 4.3-Mb region on mouse chromosome 14 that contains four clusters of genes separated by gene “deserts.” In nuclei, this region forms multiple, nonrandom “higher order” structures. These structures are based on the gene distribution pattern in primary sequence and are marked by preferential associations among multiple gene clusters. Associating gene clusters represent expressed chromatin, but their aggregation is not simply dependent on ongoing transcription. In chromosomes with aggregated gene clusters, gene deserts preferentially align with the nuclear periphery, providing evidence for chromosomal region architecture by specific associations with functional nuclear domains. Together, these data suggest dynamic, probabilistic 3D folding states for a contiguous megabase-scale chromosomal region, supporting the diverse activities of multiple genes and their conserved primary sequence organization.

Publisher

Rockefeller University Press

Subject

Cell Biology

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