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人类 V(D)J 重组中时间上不偶联的信号和编码联合形成。

Temporally uncoupled signal and coding joint formation in human V(D)J recombination.

机构信息

USC Norris Comprehensive Cancer Ctr., Department of Urology, Los Angeles, CA, 90089, United States.

USC Norris Comprehensive Cancer Ctr., Departments of Pathology, Biochemistry & Molecular Biology, Molecular Microbiology & Immunology, University of Southern California Keck School of Medicine, Molecular and Computational Biology Program, Department of Biological Sciences, 1441 Eastlake Ave., Rm. 5428, Los Angeles, CA, 90089-9176, United States.

出版信息

Mol Immunol. 2020 Dec;128:227-234. doi: 10.1016/j.molimm.2020.10.010. Epub 2020 Nov 3.

Abstract

In vertebrate antigen receptor gene rearrangement, V(D)J recombination events can occur by deletion or by inversion. For deletional events, the signal joint is deleted from the genome. Nearly half of the immunoglobulin light chain genes undergo V(D)J recombination in an inversional manner, and both signal and coding joint formation must occur to retain chromosomal integrity. But given the undetermined amount of pre-B and pre-T cell death that occurs during V(D)J recombination, the efficiency with which both joints are completed is not known, nor is the relative efficiency (balance) of signal versus coding joint formation. Signal joint formation only requires Ku and XRCC4:DNA ligase 4 of the nonhomologous DNA end joining repair pathway. Coding joint formation requires these proteins as well, but in addition requires Artemis and DNA-dependent protein kinase to open the hairpin DNA coding ends, which the RAG complex generated; and further processing is required because the hairpin opening generates incompatible 3' overhangs. Mutations in some of the end processing enzymes affect one, but only minimally the other joint. We have devised a precise cellular assay that does not have any cellular, enzymatic or biochemical selective bias to assess signal and coding joint formation independently, and it can detect intermediates for which one joint has formed but not the other. We find that intermediates with only one completed joint are more abundant than molecules with both joints completed. This indicates that either joint can form independent of the other and joint formation can be a relatively slow process.

摘要

在脊椎动物抗原受体基因重排中,V(D)J 重组事件可以通过缺失或倒位发生。对于缺失事件,信号接头从基因组中缺失。几乎一半的免疫球蛋白轻链基因以倒位的方式发生 V(D)J 重组,并且必须形成信号和编码接头以保持染色体完整性。但是,考虑到在 V(D)J 重组过程中发生的未确定数量的前 B 和前 T 细胞死亡,两个接头都完成的效率是未知的,信号与编码接头形成的相对效率(平衡)也是未知的。信号接头的形成仅需要非同源 DNA 末端连接修复途径的 Ku 和 XRCC4:DNA 连接酶 4。编码接头的形成除了需要这些蛋白质外,还需要 Artemis 和 DNA 依赖性蛋白激酶来打开 RAG 复合物产生的发夹状 DNA 编码末端,并且需要进一步的加工,因为发夹打开会产生不兼容的 3'突出端。一些末端加工酶的突变会影响一个接头,但仅对另一个接头产生最小的影响。我们设计了一种精确的细胞测定法,它不会对信号和编码接头的形成产生任何细胞、酶或生化选择性偏见,并且可以独立检测已经形成一个接头但未形成另一个接头的中间产物。我们发现只有一个完成的接头的中间产物比两个接头都完成的分子更丰富。这表明,一个接头可以独立于另一个接头形成,并且接头的形成可能是一个相对较慢的过程。

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