Systematic decoding of cis gene regulation defines context-dependent control of the multi-gene costimulatory receptor locus in human T cells

Author:

Mowery Cody T.,Freimer Jacob W.ORCID,Chen Zeyu,Casaní-Galdón SalvadorORCID,Umhoefer Jennifer M.,Arce Maya M.ORCID,Gjoni Ketrin,Daniel BenceORCID,Sandor KatalinORCID,Gowen Benjamin G.,Nguyen Vinh,Simeonov Dimitre R.,Garrido Christian M.,Curie Gemma L.,Schmidt RalfORCID,Steinhart Zachary,Satpathy Ansuman T.ORCID,Pollard Katherine S.,Corn Jacob E.ORCID,Bernstein Bradley E.,Ye Chun JimmieORCID,Marson AlexanderORCID

Abstract

AbstractCis-regulatory elements (CREs) interact with trans regulators to orchestrate gene expression, but how transcriptional regulation is coordinated in multi-gene loci has not been experimentally defined. We sought to characterize the CREs controlling dynamic expression of the adjacent costimulatory genes CD28, CTLA4 and ICOS, encoding regulators of T cell-mediated immunity. Tiling CRISPR interference (CRISPRi) screens in primary human T cells, both conventional and regulatory subsets, uncovered gene-, cell subset- and stimulation-specific CREs. Integration with CRISPR knockout screens and assay for transposase-accessible chromatin with sequencing (ATAC-seq) profiling identified trans regulators influencing chromatin states at specific CRISPRi-responsive elements to control costimulatory gene expression. We then discovered a critical CCCTC-binding factor (CTCF) boundary that reinforces CRE interaction with CTLA4 while also preventing promiscuous activation of CD28. By systematically mapping CREs and associated trans regulators directly in primary human T cell subsets, this work overcomes longstanding experimental limitations to decode context-dependent gene regulatory programs in a complex, multi-gene locus critical to immune homeostasis.

Publisher

Springer Science and Business Media LLC

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