Live imaging and biophysical modeling support a button-based mechanism of somatic homolog pairing in Drosophila
3D eukaryotic genome organization provides the structural basis for gene regulation. In Drosophila melanogaster, genome folding is characterized by somatic homolog pairing, where homologous chromosomes are intimately paired from end to end; however, how homologs identify one another and pair has rem...
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Zusammenfassung: | 3D eukaryotic genome organization provides the structural basis for gene
regulation. In Drosophila melanogaster, genome folding is characterized by
somatic homolog pairing, where homologous chromosomes are intimately
paired from end to end; however, how homologs identify one another and
pair has remained mysterious. Recently, this process has been proposed to
be driven by specifically interacting 'buttons' encoded along
chromosomes. Here, we turned this hypothesis into a quantitative
biophysical model to demonstrate that a button-based mechanism can lead to
chromosome-wide pairing. We tested our model using live-imaging
measurements of chromosomal loci tagged with the MS2 and PP7 nascent RNA
labeling systems. We show solid agreement between model predictions and
experiments in the pairing dynamics of individual homologous loci. Our
results strongly support a button-based mechanism of somatic homolog
pairing in Drosophila and provide a theoretical framework for revealing
the molecular identity and regulation of buttons. |
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DOI: | 10.5061/dryad.3j9kd51j5 |