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IG and TR single chain fragment variable (scFv) sequence analysis: a new advanced functionality of IMGT/V-QUEST and IMGT/HighV-QUEST

机译:IG和TR单链片段变量(scFv)序列分析:IMGT / V-QUEST和IMGT / HighV-QUEST的新高级功能

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Background IMGT?, the international ImMunoGeneTics information system? ( http://www.imgt.org ), was created in 1989 in Montpellier, France (CNRS and Montpellier University) to manage the huge and complex diversity of the antigen receptors, and is at the origin of immunoinformatics, a science at the interface between immunogenetics and bioinformatics. Immunoglobulins (IG) or antibodies and T cell receptors (TR) are managed and described in the IMGT? databases and tools at the level of receptor, chain and domain. The analysis of the IG and TR variable (V) domain rearranged nucleotide sequences is performed by IMGT/V-QUEST (online since 1997, 50 sequences per batch) and, for next generation sequencing (NGS), by IMGT/HighV-QUEST, the high throughput version of IMGT/V-QUEST (portal begun in 2010, 500,000 sequences per batch). In vitro combinatorial libraries of engineered antibody single chain Fragment variable (scFv) which mimic the in vivo natural diversity of the immune adaptive responses are extensively screened for the discovery of novel antigen binding specificities. However the analysis of NGS full length scFv (~850?bp) represents a challenge as they contain two V domains connected by a linker and there is no tool for the analysis of two V domains in a single chain. Methods The functionality "Analyis of single chain Fragment variable (scFv)" has been implemented in IMGT/V-QUEST and, for NGS, in IMGT/HighV-QUEST for the analysis of the two V domains of IG and TR scFv. It proceeds in five steps: search for a first closest V-REGION, full characterization of the first V-(D)-J-REGION, then search for a second V-REGION and full characterization of the second V-(D)-J-REGION, and finally linker delimitation. Results For each sequence or NGS read, positions of the 5′V-DOMAIN, linker and 3′V-DOMAIN in the scFv are provided in the ‘V-orientated’ sense. Each V-DOMAIN is fully characterized (gene identification, sequence description, junction analysis, characterization of mutations and amino changes). The functionality is generic and can analyse any IG or TR single chain nucleotide sequence containing two V domains, provided that the corresponding species IMGT reference directory is available. Conclusion The “Analysis of single chain Fragment variable (scFv)” implemented in IMGT/V-QUEST and, for NGS, in IMGT/HighV-QUEST provides the identification and full characterization of the two V domains of full-length scFv (~850?bp) nucleotide sequences from combinatorial libraries. The analysis can also be performed on concatenated paired chains of expressed antigen receptor IG or TR repertoires.
机译:背景IMGT ?,国际ImMunoGeneTics信息系统? (http://www.imgt.org)于1989年在法国蒙彼利埃(CNRS和蒙彼利埃大学)创立,以管理抗原受体的巨大而复杂的多样性,是免疫信息学的起源。免疫遗传学和生物信息学之间的接口。免疫球蛋白(IG)或抗体和T细胞受体(TR)在IMGT?中进行管理和描述。受体,链和域级别的数据库和工具。 IG和TR可变(V)域重排的核苷酸序列的分析由IMGT / V-QUEST(自1997年以来在线,每批50个序列)进行;对于下一代测序(NGS),由IMGT / HighV-QUEST进行, IMGT / V-QUEST的高通量版本(门户于2010年开始,每批500,000个序列)。广泛筛选了模拟免疫适应性反应的体内自然多样性的工程化抗体单链片段变量(scFv)的体外组合文库,以发现新的抗原结合特异性。但是,NGS全长scFv(〜850?bp)的分析面临挑战,因为它们包含两个通过接头连接的V结构域,并且没有用于分析单链中两个V结构域的工具。方法已在IMGT / V-QUEST中实现了“单链片段变量(scFv)分析”功能;对于NGS,在IMGT / HighV-QUEST中实现了功能,以分析IG和TR scFv的两个V域。它分五个步骤进行:搜索第一个最接近的V-REGION,第一个V-(D)-J-REGION的完整特征,然后搜索第二个V-REGION和第二个V-(D)-的完整特征J-REGION,最后是链接程序定界。结果对于每个序列或读取的NGS,scFv中5'V-DOMAIN,接头和3'V-DOMAIN的位置均以“ V向”的方式提供。每个V-DOMAIN都具有完整的特征(基因鉴定,序列描述,连接分析,突变和氨基酸变化的特征)。该功能是通用的,并且可以分析包含两个V结构域的任何IG或TR单链核苷酸序列,前提是相应的物种IMGT参考目录可用。结论在IMGT / V-QUEST和NGS中在IMGT / HighV-QUEST中实施的“单链片段变量(scFv)分析”提供了全长scFv(〜850)的两个V结构域的鉴定和完整表征。来自组合文库的核苷酸序列)。还可以对表达的抗原受体IG或TR组成部分的串联配对链进行分析。

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