Nuclear organization of active and inactive chromatin domains uncovered by chromosome conformation capture–on-chip (4C)

M Simonis, P Klous, E Splinter, Y Moshkin… - Nature …, 2006 - nature.com
M Simonis, P Klous, E Splinter, Y Moshkin, R Willemsen, E De Wit, B Van Steensel
Nature genetics, 2006nature.com
The spatial organization of DNA in the cell nucleus is an emerging key contributor to
genomic function,,,,,,,,,,,. We developed 4C technology (chromosome conformation capture
(3C)-on-chip), which allows for an unbiased genome-wide search for DNA loci that contact a
given locus in the nuclear space. We demonstrate here that active and inactive genes are
engaged in many long-range intrachromosomal interactions and can also form
interchromosomal contacts. The active β-globin locus in fetal liver preferentially contacts …
Abstract
The spatial organization of DNA in the cell nucleus is an emerging key contributor to genomic function,,,,,,,,,,,. We developed 4C technology (chromosome conformation capture (3C)-on-chip), which allows for an unbiased genome-wide search for DNA loci that contact a given locus in the nuclear space. We demonstrate here that active and inactive genes are engaged in many long-range intrachromosomal interactions and can also form interchromosomal contacts. The active β-globin locus in fetal liver preferentially contacts transcribed, but not necessarily tissue-specific, loci elsewhere on chromosome 7, whereas the inactive locus in fetal brain contacts different transcriptionally silent loci. A housekeeping gene in a gene-dense region on chromosome 8 forms long-range contacts predominantly with other active gene clusters, both in cis and in trans, and many of these intra- and interchromosomal interactions are conserved between the tissues analyzed. Our data demonstrate that chromosomes fold into areas of active chromatin and areas of inactive chromatin and establish 4C technology as a powerful tool to study nuclear architecture.
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