Litcius/Paper detail

Cell-type-specific loops linked to RNA polymerase II elongation in human neural differentiation

Katelyn R. Titus, Zoltán Simándi, Harshini Chandrashekar, Dominik Paquet, Jennifer E. Phillips‐Cremins

2024Cell Genomics12 citationsDOIOpen Access PDF

Abstract

DNA is folded into higher-order structures that shape and are shaped by genome function. The role of long-range loops in the establishment of new gene expression patterns during cell fate transitions remains poorly understood. Here, we investigate the link between cell-specific loops and RNA polymerase II (RNA Pol II) during neural lineage commitment. We find thousands of loops decommissioned or gained de novo upon differentiation of human induced pluripotent stem cells (hiPSCs) to neural progenitor cells (NPCs) and post-mitotic neurons. During hiPSC-to-NPC and NPC-to-neuron transitions, genes changing from RNA Pol II initiation to elongation are >4-fold more likely to anchor cell-specific loops than repressed genes. Elongated genes exhibit significant mRNA upregulation when connected in cell-specific promoter-enhancer loops but not invariant promoter-enhancer loops or promoter-promoter loops or when unlooped. Genes transitioning from repression to RNA Pol II initiation exhibit a slight mRNA increase independent of loop status. Our data link cell-specific loops and robust RNA Pol II-mediated elongation during neural cell fate transitions.

Topics & Concepts

BiologyEnhancerRNARNA polymerase IIMolecular biologyCell biologyGeneInduced pluripotent stem cellNeural stem cellGene expressionGeneticsPromoterStem cellEmbryonic stem cellGenomics and Chromatin DynamicsRNA Research and SplicingPlant Molecular Biology Research