Skip to main content
Search
Main content
Sci Adv
Published

Three-dimensional chromatin interactions remain stable upon CAG/CTG repeat expansion.

Authors

Gustavo A Ruiz Buendía, Marion Leleu, Flavia Marzetta, Ludovica Vanzan, Jennifer Y Tan, Victor Ythier, Emma L Randall, Ana C Marques, Tuncay Baubec, Rabih Murr, Ioannis Xenarios, Vincent Dion

Abstract

Expanded CAG/CTG repeats underlie 13 neurological disorders, including myotonic dystrophy type 1 (DM1) and Huntington's disease (HD). Upon expansion, disease loci acquire heterochromatic characteristics, which may provoke changes to chromatin conformation and thereby affect both gene expression and repeat instability. Here, we tested this hypothesis by performing 4C sequencing at the DMPK and HTT loci from DM1 and HD-derived cells. We find that allele sizes ranging from 15 to 1700 repeats displayed similar chromatin interaction profiles. This was true for both loci and for alleles with different DNA methylation levels and CTCF binding. Moreover, the ectopic insertion of an expanded CAG repeat tract did not change the conformation of the surrounding chromatin. We conclude that CAG/CTG repeat expansions are not enough to alter chromatin conformation in cis. Therefore, it is unlikely that changes in chromatin interactions drive repeat instability or changes in gene expression in these disorders.

PMID:32656337 | DOI:10.1126/sciadv.aaz4012

UK DRI Authors

Vincent Dion

Prof Vincent Dion

Group Leader

Developing new treatments to stop the progression of expanded repeat disorders

Prof Vincent Dion