Author:
Parteka-Tojek Zofia,Zhu Jacqueline Jufen,Lee Byoungkoo,Jodkowska Karolina,Wang Ping,Aaron Jesse,Chew Teng-Leong,Banecki Krzysztof,Plewczynski Dariusz,Ruan Yijun
Abstract
AbstractThe three-dimensional (3D) genome structure plays a fundamental role in gene regulation and cellular functions. Recent studies in 3D genomics inferred the very basic functional chromatin folding structures known as chromatin loops, the long-range chromatin interactions that are mediated by protein factors and dynamically extruded by cohesin. We combined the use of FISH staining of a very short (33 kb) chromatin fragment, interferometric photoactivated localization microscopy (iPALM), and traveling salesman problem-based heuristic loop reconstruction algorithm from an image of the one of the strongest CTCF-mediated chromatin loops in human lymphoblastoid cells. In total, we have generated thirteen good quality images of the target chromatin region with 2–22 nm oligo probe localization precision. We visualized the shape of the single chromatin loops with unprecedented genomic resolution which allowed us to study the structural heterogeneity of chromatin looping. We were able to compare the physical distance maps from all reconstructed image-driven computational models with contact frequencies observed by ChIA-PET and Hi-C genomic-driven methods to examine the concordance between single cell imaging and population based genomic data.
Funder
Polish National Science Centre
Politechnika Warszawska
Polish Ministry of Science and Higher Education
Fundacja na rzecz Nauki Polskiej
NIH
European Commission
Publisher
Springer Science and Business Media LLC
Cited by
12 articles.
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