Convergent transcription at intragenic super-enhancers targets AID-initiated genomic instability

基因内超增强子的聚合转录靶向AID引发的基因组不稳定性

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作者:Fei-Long Meng, Zhou Du, Alexander Federation, Jiazhi Hu, Qiao Wang, Kyong-Rim Kieffer-Kwon, Robin M Meyers, Corina Amor, Caitlyn R Wasserman, Donna Neuberg, Rafael Casellas, Michel C Nussenzweig, James E Bradner, X Shirley Liu, Frederick W Alt
期刊:Cell影响因子:45.500
时间:2014起止号:2014 Dec 18;159(7):1538-48.
doi:10.1016/j.cell.2014.11.014研究方向: 信号转导

Abstract

Activation-induced cytidine deaminase (AID) initiates both somatic hypermutation (SHM) for antibody affinity maturation and DNA breakage for antibody class switch recombination (CSR) via transcription-dependent cytidine deamination of single-stranded DNA targets. Though largely specific for immunoglobulin genes, AID also acts on a limited set of off-targets, generating oncogenic translocations and mutations that contribute to B cell lymphoma. How AID is recruited to off-targets has been a long-standing mystery. Based on deep GRO-seq studies of mouse and human B lineage cells activated for CSR or SHM, we report that most robust AID off-target translocations occur within highly focal regions of target genes in which sense and antisense transcription converge. Moreover, we found that such AID-targeting "convergent" transcription arises from antisense transcription that emanates from super-enhancers within sense transcribed gene bodies. Our findings provide an explanation for AID off-targeting to a small subset of mostly lineage-specific genes in activated B cells.

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