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Literature DB >> 27637145

Multi-tiered Reorganization of the Genome during B Cell Affinity Maturation Anchored by a Germinal Center-Specific Locus Control Region.

Karen L Bunting¹, T David Soong², Rajat Singh³, Yanwen Jiang⁴, Wendy Béguelin⁵, David W Poloway⁵, Brandon L Swed⁵, Katerina Hatzi⁵, William Reisacher⁶, Matt Teater⁷, Olivier Elemento⁸, Ari M Melnick⁹.

Abstract

During the humoral immune response, B cells undergo a dramatic change in phenotype to enable antibody affinity maturation in germinal centers (GCs). Using genome-wide chromosomal conformation capture (Hi-C), we found that GC B cells undergo massive reorganization of the genomic architecture that encodes the GC B cell transcriptome. Coordinate expression of genes that specify the GC B cell phenotype-most prominently BCL6-was achieved through a multilayered chromatin reorganization process involving (1) increased promoter connectivity, (2) formation of enhancer networks, (3) 5' to 3' gene looping, and (4) merging of gene neighborhoods that share active epigenetic marks. BCL6 was an anchor point for the formation of GC-specific gene and enhancer loops on chromosome 3. Deletion of a GC-specific, highly interactive locus control region upstream of Bcl6 abrogated GC formation in mice. Thus, large-scale and multi-tiered genomic three-dimensional reorganization is required for coordinate expression of phenotype-driving gene sets that determine the unique characteristics of GC B cells.

Entities: CellLine Chemical Disease Gene Species

Mesh：

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Year: 2016 PMID： 27637145 PMCID： PMC5033726 DOI： 10.1016/j.immuni.2016.08.012

Source DB: PubMed Journal: Immunity ISSN： 1074-7613 Impact factor: 31.745

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