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Kabat Database and its applications: 30 years after the first variability plot

机译:Kabat数据库及其应用程序:第一个变异图绘制30年后

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摘要

The Kabat Database was initially started in 1970 to determine the combining site of antibodies based on the available amino acid sequences at that time. Bence Jones proteins, mostly from human, were aligned, using the now-known Kabat numbering system, and a quantitative measure, variability, was calculated for every position. Three peaks, at positions 24–34, 50–56 and 89–97, were identified and proposed to form the complementarity determining regions (CDR) of light chains. Subsequently, antibody heavy chain amino acid sequences were also aligned using a different numbering system, since the locations of their CDRs (31–35B, 50–65 and 95–102) are different from those of the light chains. CDRL1 starts right after the first invariant Cys 23 of light chains, while CDRH1 is eight amino acid residues away from the first invariant Cys 22 of heavy chains. During the past 30 years, the Kabat database has grown to include nucleotide sequences, sequences of T cell receptors for antigens (TCR), major histocompatibility complex (MHC) class I and II molecules and other proteins of immunological interest. It has been used extensively by immunologists to derive useful structural and functional information from the primary sequences of these proteins. An overall view of the Kabat Database and its various applications are summarized here. The Kabat Database is freely available at http://immuno.bme.nwu.edu
机译:Kabat数据库最初于1970年启动,用于根据当时可用的氨基酸序列确定抗体的结合位点。使用现在已知的Kabat编号系统,对大多数来自人类的Bence Jones蛋白进行了比对,并计算了每个位置的定量度量(变异性)。确定并提出了在位置24–34、50–56和89–97处的三个峰,以形成轻链的互补决定区(CDR)。随后,抗体重链氨基酸序列也使用不同的编号系统进行比对,因为其CDR的位置(31–35B,50–65和95–102)不同于轻链。 CDRL1在轻链的第一个恒定Cys 23之后立即开始,而CDRH1与重链的第一个恒定Cys 22相距八个氨基酸残基。在过去的30年中,Kabat数据库不断发展壮大,包括核苷酸序列,抗原T细胞受体序列(TCR),主要组织相容性复合体(MHC)I和II类分子以及其他具有免疫学意义的蛋白质。免疫学家已广泛使用它来从这些蛋白质的主要序列中获得有用的结构和功能信息。这里总结了Kabat数据库及其各种应用程序的整体视图。 Kabat数据库可从http://immuno.bme.nwu.edu免费获得。

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