Sequence-Dependent Dynamics of Synthetic and Endogenous RSSs in V(D)J Recombination

Hirokawa, Soichi; Chure, Griffin; Belliveau, Nathan M.; Lovely, Geoffrey A.; Anaya, Michael; Schatz, David G.; Baltimore, David; Phillips, Rob

doi:10.1101/791954

Cited by 3 publications

(2 citation statements)

References 53 publications

(101 reference statements)

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“…Recently, a research reported cryoelectron microscopy structures of synaptic RAG complexes at up to 3.4 Å resolution, which reveal a closed conformation with base flipping and base-specific recognition of RSSs (Ru et al, 2015). Another study employed a single-molecule method to track the RAG-RSS interaction, which can provide a relatived complete kinetic description of the initial phases of V(D)J recombination (Hirokawa et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

The Usage of Human IGHJ Genes Follows a Particular Non-random Selection: The Recombination Signal Sequence May Affect the Usage of Human IGHJ Genes

Shu

Dong

et al. 2020

Front. Genet.

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The formation of the B cell receptor (BCR) heavy chain variable region is derived from the germline V(D)J gene rearrangement according to the “12/23” rule and the “beyond 12/23” rule. The usage frequency of each V(D)J gene in the peripheral BCR repertoires is related to the initial recombination, self-tolerance selection, and the clonal proliferative response. However, their specific differences and possible mechanisms are still unknown. We analyzed in-frame and out-of-frame BCR-H repertoires from human samples with normal physiological and various pathological conditions by high-throughput sequencing. Our results showed that IGHJ gene frequency follows a similar pattern which is previously known, where IGHJ4 is used at high frequency (>40%), IGHJ6/IGHJ3/IGHJ5 is used at medium frequencies (10∼20%), and IGH2/IGHJ1 is used at low frequency (<4%) under whether normal physiological or various pathological conditions. However, our analysis of the recombination signal sequences suggested that the conserved non-amer and heptamer and certain 23 bp spacer length may affect the initial IGHD-IGHJ recombination, which results in different frequencies of IGHJ genes among the initial BCR-H repertoire. Based on this “initial repertoire,” we recommend that re-evaluation and further investigation are needed when analyzing the significance and mechanism of IGHJ gene frequency in self-tolerance selection and the clonal proliferative response.

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Section: Introductionmentioning

confidence: 99%

The Usage of Human IGHJ Genes Follows a Particular Non-random Selection: The Recombination Signal Sequence May Affect the Usage of Human IGHJ Genes

Shu

Dong

et al. 2020

Front. Genet.

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“…RAG recognizes conserved recombination signal sequences (RSSs) positioned adjacent to V, D, and J gene segments. A bona fide RSS contains a conserved palindromic heptamer (consensus 5′-CACAGTG) and A-rich nonamer (consensus 5′-ACAAAAACC) separated by a degenerate spacer of either 12 or 23 base pairs (Hirokawa, et al,2020;Schatz and Ji,2011). The process of efficient recombination is contingent upon the presence of recombination signal sequences (RSSs) with differing spacer lengths, as dictated by the "12/23 rule" (Banerjee and Schatz,2014;Eastman, et al,1996;Shi, et al,2020).…”

Section: Introductionmentioning

confidence: 99%

RAG1 and RAG2 Non-core Regions Are Implicated in Leukemogenesis and Off-target V(D)J Recombination in BCR-ABL1-driven B-cell Lineage Lym-phoblastic Leukemia

Yu,

Zhou,

Chen

et al. 2023

Preprint

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The evolutionary conservation of non-core RAG regions suggests significant roles that might involve quantitative or qualitative alterations in RAG activity. Off-target V(D)J recombination contributes to lymphomagenesis and is exacerbated by RAG2’ C-terminus absence in Tp53-/-mice thymic lymphomas. However, the genomic stability effects of non-core regions from both cRAG1 and cRAG2 inBCR-ABL1+B-lymphoblastic leukemia (BCR-ABL1+B-ALL), the characteristics, and mechanisms of non-core regions in suppressing off-target V(D)J recombination remains unclear. Here, we established three mice models ofBCR-ABL1+B-ALL infull-length RAG(fRAG),core RAG1(cRAG1), andcore RAG2(cRAG2) mice. ThecRAG(cRAG1 and cRAG2) leukemia cells exhibited greatr malignant tumor characteristics compared tofRAGcells. Additionally,cRAGcells showed higher frequency of off-target V(D)J recombination and oncogenic mutations thanfRAG. We also revealed decreased RAG binding accuracy incRAGcells and a smaller recombinant size incRAG1cells, which could potentially exacerbate off-target V(D)J recombination incRAGcells. In conclusion, these findings indicate that the non-core RAG regions, particularly the non-core region of RAG1, play a significant role in preserving V(D)J recombination precision and genomic stability inBCR-ABL1+B-ALL.

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Sequence-Dependent Dynamics of Synthetic and Endogenous RSSs in V(D)J Recombination

Cited by 3 publications

References 53 publications

The Usage of Human IGHJ Genes Follows a Particular Non-random Selection: The Recombination Signal Sequence May Affect the Usage of Human IGHJ Genes

The Usage of Human IGHJ Genes Follows a Particular Non-random Selection: The Recombination Signal Sequence May Affect the Usage of Human IGHJ Genes

RAG1 and RAG2 Non-core Regions Are Implicated in Leukemogenesis and Off-target V(D)J Recombination in BCR-ABL1-driven B-cell Lineage Lym-phoblastic Leukemia

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