Author
Listed:
- Daniel S. Park
(University of Pennsylvania
University of Pennsylvania)
- Son C. Nguyen
(University of Pennsylvania
University of Pennsylvania)
- Randi Isenhart
(University of Pennsylvania
University of Pennsylvania)
- Parisha P. Shah
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Wonho Kim
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- R. Jordan Barnett
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Aditi Chandra
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Jennifer M. Luppino
(University of Pennsylvania
University of Pennsylvania)
- Jailynn Harke
(University of Pennsylvania
University of Pennsylvania)
- May Wai
(University of Pennsylvania
University of Pennsylvania)
- Patrick J. Walsh
(University of Pennsylvania
University of Pennsylvania)
- Richard J. Abdill
(University of Pennsylvania
University of Pennsylvania)
- Rachel Yang
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Yemin Lan
(University of Pennsylvania)
- Sora Yoon
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Rebecca Yunker
(University of Pennsylvania
University of Pennsylvania)
- Masato T. Kanemaki
(National Institute of Genetics, Research Organization of Information and Systems (ROIS)
The Graduate University for Advanced Studies (SOKENDAI)
The University of Tokyo)
- Golnaz Vahedi
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Jennifer E. Phillips-Cremins
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Rajan Jain
(University of Pennsylvania
University of Pennsylvania
University of Pennsylvania
University of Pennsylvania)
- Eric F. Joyce
(University of Pennsylvania
University of Pennsylvania)
Abstract
The human genome functions as a three-dimensional chromatin polymer, driven by a complex collection of chromosome interactions1–3. Although the molecular rules governing these interactions are being quickly elucidated, relatively few proteins regulating this process have been identified. Here, to address this gap, we developed high-throughput DNA or RNA labelling with optimized Oligopaints (HiDRO)—an automated imaging pipeline that enables the quantitative measurement of chromatin interactions in single cells across thousands of samples. By screening the human druggable genome, we identified more than 300 factors that influence genome folding during interphase. Among these, 43 genes were validated as either increasing or decreasing interactions between topologically associating domains. Our findings show that genetic or chemical inhibition of the ubiquitous kinase GSK3A leads to increased long-range chromatin looping interactions in a genome-wide and cohesin-dependent manner. These results demonstrate the importance of GSK3A signalling in nuclear architecture and the use of HiDRO for identifying mechanisms of spatial genome organization.
Suggested Citation
Daniel S. Park & Son C. Nguyen & Randi Isenhart & Parisha P. Shah & Wonho Kim & R. Jordan Barnett & Aditi Chandra & Jennifer M. Luppino & Jailynn Harke & May Wai & Patrick J. Walsh & Richard J. Abdill, 2023.
"High-throughput Oligopaint screen identifies druggable 3D genome regulators,"
Nature, Nature, vol. 620(7972), pages 209-217, August.
Handle:
RePEc:nat:nature:v:620:y:2023:i:7972:d:10.1038_s41586-023-06340-w
DOI: 10.1038/s41586-023-06340-w
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