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The RAG-HMG1 Complex Enforces the 12/23 Rule of V(D)J Recombination Specifically at the Double-Hairpin Formation Step

机译:RAG-HMG1复合体在双发夹形成步骤特别是强化了V(D)J重组的12/23规则

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摘要

A central unanswered question concerning the initial phases of V(D)J recombination has been at which step the 12/23 rule applies. This rule, which governs which variable (V), diversity (D), and joining (J) segments are able to pair during recombination, could operate at the level of signal sequence synapsis after RAG-HMG1 complex binding, signal nicking, or signal hairpin formation. It has also been unclear whether additional proteins are required to achieve adherence to the 12/23 rule. We developed a novel system for the detailed biochemical analysis of the 12/23 rule by using an oligonucleotide-based substrate that can include two signals. Under physiologic conditions, we found that the complex of RAG1, RAG2, and HMG1 can successfully recapitulate the 12/23 rule with the same specificity as that seen intracellularly and in crude extracts. The cleavage complex can bind and nick 12×12 and 23×23 substrates as well as 12×23 substrates. However, hairpin formation occurs at both of the signals only on 12×23 substrates. Moreover, under physiologic conditions, the presence of a partner 23-bp spacer suppresses single-site hairpin formation at a 12-bp spacer and vice versa. Hence, this study illustrates that synapsis suppresses single-site reactions, thereby explaining the high physiologic ratio of paired versus unpaired V(D)J recombination events in lymphoid cells.
机译:有关V(D)J重组初始阶段的一个未解决的中心问题是在哪个步骤应用12/23规则。该规则控制重组期间可变(V),多样性(D)和连接(J)片段能够配对的规则,可以在RAG-HMG1复杂结合,信号切口或信号产生后在信号序列突触水平起作用发夹的形成。还不清楚是否需要额外的蛋白质来实现遵守12/23规则。我们开发了一种新型系统,用于通过使用可包含两个信号的基于寡核苷酸的底物对12/23法则进行详细的生化分析。在生理条件下,我们发现RAG1,RAG2和HMG1的复合物可以成功地概括12/23规则,其特异性与在细胞内和在粗提物中所见的特异性相同。切割复合物可以结合并划痕12×12和23×23底物以及12×23底物。但是,发夹形成仅在12×23基板上的两个信号处发生。此外,在生理条件下,伴侣23 bp间隔基的存在会抑制12 bp间隔基上的单点发夹形成,反之亦然。因此,这项研究表明突触抑制了单点反应,从而解释了淋巴样细胞中成对与不成对的V(D)J重组事件的高生理比率。

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