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首页> 外文期刊>Archivum Immunologiae et Therapiae Experimentalis >The roles of the RAG1 and RAG2 “non-core” regions in V(D)J recombination and lymphocyte development
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The roles of the RAG1 and RAG2 “non-core” regions in V(D)J recombination and lymphocyte development

机译:RAG1和RAG2“非核心”区域在V(D)J重组和淋巴细胞发育中的作用

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摘要

The enormous repertoire of the vertebrate specific immune system relies on the rearrangement of discrete gene segments into intact antigen receptor genes during the early stages of B-and T-cell development. This V(D)J recombination is initiated by a lymphoid-specific recombinase comprising the RAG1 and RAG2 proteins, which introduces double-strand breaks in the DNA adjacent to the coding segments. Much of the biochemical research into V(D)J recombination has focused on truncated or “core” fragments of RAG1 and RAG2, which lack approximately one third of the amino acids from each. However, genetic analyses of SCID and Omenn syndrome patients indicate that residues outside the cores are essential to normal immune development. This is in agreement with the striking degree of conservation across all vertebrate classes in certain non-core domains. Work from multiple laboratories has shed light on activities resident within these domains, including ubiquitin ligase activity and KPNA1 binding by the RING finger domain of RAG1 and the recognition of specific chromatin modifications as well as phosphoinositide binding by the PHD module of RAG2. In addition, elements outside of the cores are necessary for regulated protein expression and turnover. Here the current state of knowledge is reviewed regarding the non-core regions of RAG1 and RAG2 and how these findings contribute to our broader understanding of recombination. Keywords V(D)J recombination - RAG1 - RAG2 - RING finger - PHD domain/plant homeodomain
机译:脊椎动物特异性免疫系统的巨大组成部分依赖于在B细胞和T细胞发育的早期将离散的基因片段重新排列为完整的抗原受体基因。这种V(D)J重组是由包含RAG1和RAG2蛋白的淋巴样特异性重组酶启动的,该酶在邻近编码段的DNA中引入双链断裂。 V(D)J重组的许多生化研究都集中在RAG1和RAG2的截短或“核心”片段上,它们各自缺少大约三分之一的氨基酸。但是,对SCID和Omenn综合征患者的遗传分析表明,核心外部的残基对于正常的免疫发育至关重要。这与某些非核心领域中所有脊椎动物类别的惊人保护程度一致。来自多个实验室的工作揭示了这些域中的固有活性,包括泛素连接酶活性和RAG1的RING指域与KPNA1的结合,以及对特定染色质修饰的识别以及RAG2的PHD模块与磷酸肌醇的结合。另外,核心以外的元素对于调节蛋白的表达和周转是必需的。在这里,我们对RAG1和RAG2的非核心区域以及这些发现如何有助于我们对重组的更广泛理解进行了综述。关键字V(D)J重组-RAG1-RAG2-无名指-PHD域/植物同源域

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