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Predicting class II MHC/peptide multi-level binding with an iterative stepwise discriminant analysis meta-algorithm.

机译:使用迭代逐步判别分析元算法预测II类MHC /肽多级结合。

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MOTIVATION: Predicting peptides that bind to both Major Histocompatibility Complex (MHC) molecules and T cell receptors provides crucial information for vaccine development. An agretope is that portion of a peptide that interacts with an MHC molecule. The identification and prediction of agretopes is the first step towards vaccine design. RESULTS: An iterative stepwise discriminant analysis meta-algorithm is utilized to derive a quantitative motif for classifying potential agretopes as high-, moderate- or non-binders for HLA-DR1, a class II MHC molecule. A large molecular online database provides the input for this data-driven algorithm. The model correctly classifies over 85% of the peptides in the database. AVAILABILITY: Stepwise discriminant analysis software is available commercially in SPSS and BMDP statistical software packages. Peptides known to bind MHC molecules can be downloaded from http://wehih.wehi.edu.au/mhcpep/. Peptides known not to bind HLA-DR1 are available from the author upon request. CONTACT: ronna
机译:动机:预测与主要组织相容性复合体(MHC)分子和T细胞受体结合的肽为疫苗开发提供重要信息。促胰液素是肽的与MHC分子相互作用的部分。鉴定和预测gregotopes是疫苗设计的第一步。结果:迭代逐步判别分析元算法被用来导出定量基元,以将潜在的类固位激素分类为II类MHC分子HLA-DR1的高,中或非结合基。大型分子在线数据库为该数据驱动算法提供了输入。该模型正确分类了数据库中85%以上的肽。可用性:逐步判别分析软件可从SPSS和BMDP统计软件包中购买。可以结合http://wehih.wehi.edu.au/mhcpep/下载已知结合MHC分子的肽。应要求,作者可提供已知不与HLA-DR1结合的肽。联系人:ronna

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