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Quantitative structure-activity relationships and the prediction of MHC supermotifs.

机译:定量构效关系和MHC超基元的预测。

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The underlying assumption in quantitative structure-activity relationship (QSAR) methodology is that related chemical structures exhibit related biological activities. We review here two QSAR methods in terms of their applicability for human MHC supermotif definition. Supermotifs are motifs that characterise binding to more than one allele. Supermotif definition is the initial in silico step of epitope-based vaccine design. The first QSAR method we review here--the additive method--is based on the assumption that the binding affinity of a peptide depends on contributions from both amino acids and the interactions between them. The second method is a 3D-QSAR method: comparative molecular similarity indices analysis (CoMSIA). Both methods were applied to 771 peptides binding to 9 HLA alleles. Five of the alleles (A*0201, A*0202, A*0203, A*0206 and A*6802) belong to the HLA-A2 superfamily and the other four (A*0301, A*1101, A*3101 and A*6801) to the HLA-A3 superfamily. For each superfamily, supermotifs defined by the two QSAR methods agree closely and are supported by many experimental data.
机译:定量构效关系(QSAR)方法的基本假设是相关的化学结构表现出相关的生物学活性。我们在这里回顾了两种QSAR方法在人类MHC超基元定义中的适用性。超基序是表征与多个等位基因结合的基序。 Supermotif的定义是基于表位的疫苗设计的计算机化第一步。我们在这里回顾的第一个QSAR方法-加成法-是基于这样的假设,即肽的结合亲和力取决于氨基酸和两者之间的相互作用的贡献。第二种方法是3D-QSAR方法:比较分子相似性指数分析(CoMSIA)。两种方法均应用于结合9个HLA等位基因的771个肽段。等位基因中的五个(A * 0201,A * 0202,A * 0203,A * 0206和A * 6802)属于HLA-A2超家族,其他四个等位基因(A * 0301,A * 1101,A * 3101和A * 6801)加入HLA-A3超家族。对于每个超家族,由两种QSAR方法定义的超基元非常一致,并得到许多实验数据的支持。

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