The mouse Igh locus is organized into a developmentally regulated topologically associated domain (TAD) that is divided into subTADs. Here we identify a series of distal V(H) enhancers (E(VH)s) that collaborate to configure the locus. E(VH)s engage in a network of long-range interactions that interconnect the subTADs and the recombination center at the D(H)J(H) gene cluster. Deletion of E(VH)1 reduces V gene rearrangement in its vicinity and alters discrete chromatin loops and higher order locus conformation. Reduction in the rearrangement of the V(H)11 gene used in anti-PtC responses is a likely cause of the observed reduced splenic B1 B cell compartment. E(VH)1 appears to block long-range loop extrusion that in turn contributes to locus contraction and determines the proximity of distant V(H) genes to the recombination center. E(VH)1 is a critical architectural and regulatory element that coordinates chromatin conformational states that favor V(D)J rearrangement.
An Igh distal enhancer modulates antigen receptor diversity by determining locus conformation.
Igh远端增强子通过决定基因座构象来调节抗原受体多样性
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作者:Bhat Khalid H, Priyadarshi Saurabh, Naiyer Sarah, Qu Xinyan, Farooq Hammad, Kleiman Eden, Xu Jeffery, Lei Xue, Cantillo Jose F, Wuerffel Robert, Baumgarth Nicole, Liang Jie, Feeney Ann J, Kenter Amy L
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2023 | 起止号: | 2023 Mar 3; 14(1):1225 |
| doi: | 10.1038/s41467-023-36414-2 | 研究方向: | 其它 |
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