Abstract : Genome-wide derivatives of the chromosome conformation capture (3C) technique are now well-established approaches to study the multiscale average organization of chromosomes from bacteria to mammals. However, the experimental parameters of the protocol have to be optimized for different species, and the downstream experimental products (i.e., pair-end sequences) are influenced by these parameters. Here, we describe a complete pipeline to generate 3C-seq libraries and compute chromosomal contact maps of yeast species.
https://hal-pasteur.archives-ouvertes.fr/pasteur-01419912
Contributor : Romain Koszul <>
Submitted on : Tuesday, May 16, 2017 - 10:01:03 AM Last modification on : Thursday, December 10, 2020 - 11:09:34 AM Long-term archiving on: : Friday, August 18, 2017 - 12:40:08 AM