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        Static Energy Analysis of MHC Class I and Class II Peptide-Binding Affinity

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        940
        Antigenic peptide is presented to a T-cell receptor (TCR) through the formation of a stable complex with a major histocompatibility complex (MHC) molecule. Various predictive algorithms have been developed to estimate a peptide’s capacity to form a stable complex with a given MHC class II allele, a technique integral to the strategy of vaccine design. These have previously incorporated such computational techniques as quantitative matrices and neural networks. A novel predictive technique is described, which uses molecular modeling of predetermined crystal structures to estimate the stability of an MHC class II–peptide complex. The structures are remodeled, energy minimized, and annealed before the energetic interaction is calculated
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