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High-Throughput Discovery and Characterization of Human Transcriptional Effectors
Author(s) -
Josh Tycko,
Nicole DelRosso,
Gaelen T. Hess,
Aradhana,
Abhimanyu Banerjee,
Adi Mukund,
Mike V. Van,
Braeden K. Ego,
David Yao,
Kaitlyn Spees,
Peter Suzuki,
Georgi K. Marinov,
Anshul Kundaje,
Michael C. Bassik,
Lacramioara Bintu
Publication year - 2020
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2020.11.024
Subject(s) - biology , repressor , effector , gene silencing , gatad2b , genetics , hox gene , computational biology , homeobox , krüppel , gene , transcription factor , microbiology and biotechnology
Thousands of proteins localize to the nucleus; however, it remains unclear which contain transcriptional effectors. Here, we develop HT-recruit, a pooled assay where protein libraries are recruited to a reporter, and their transcriptional effects are measured by sequencing. Using this approach, we measure gene silencing and activation for thousands of domains. We find a relationship between repressor function and evolutionary age for the KRAB domains, discover that Homeodomain repressor strength is collinear with Hox genetic organization, and identify activities for several domains of unknown function. Deep mutational scanning of the CRISPRi KRAB maps the co-repressor binding surface and identifies substitutions that improve stability/silencing. By tiling 238 proteins, we find repressors as short as ten amino acids. Finally, we report new activator domains, including a divergent KRAB. These results provide a resource of 600 human proteins containing effectors and demonstrate a scalable strategy for assigning functions to protein domains.

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