识别蛔虫病主要组织相容性复合体结合抗原肽的计算方法

S. Mishra, G. Vs
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引用次数: 1

摘要

类蛔虫引起人类“蛔虫病”,其消除是公众关注的主要问题。在目前的研究中,我们用PSSM(位置特定评分矩阵)和SVM(支持向量机)算法等计算方法预测了MHC(主要组织相容性复合体)I类和II类结合肽。我们预测蛔虫线粒体色素b蛋白与mhc - 1分子的肽结合物分别为11mer_H2_Db、10mer_H2_Db、9mer_H2_Db、8mer_H2_Db。同时研究了MHC I类肽结合的综合预测;利用氨基酸的序列和性质研究蛋白酶体C端裂解和TAP的转运效率。我们还利用位置特异性评分矩阵发现了多肽与不同等位基因的结合。细胞色素B来自蛔虫(365个残基长),有357个具有抗原MHC结合肽的名字。基于PSSM的服务器将预测从序列到MHCII分子的肽结合物为I_Ab。p, I_Ad。p, I_Ag7,这是蛔虫细胞色素B的抗原表位区域。这项研究有助于合理设计疫苗,同时增加对免疫系统抗抗原作用的认识。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Computational Approach to Identify the Major Histocompatibility Complex Binding Antigenic Peptides from ‘Ascariasis’
The Ascaris lumbricoides cause ‘ascariasis’ in human and its elimination is the major public concern. In this current investigation, we predicted the MHC (Major Histocompatibility Complex) class I & II binding peptides with computational approach like PSSM (Position Specific Scoring Matrices) and SVM (Support Vector Machine) algorithms. We predict the peptide binders of Cytochrome b (mitochondrion) protein from Ascaris lumbricoide sequence to MHC-I molecules are as 11mer_H2_Db, 10mer_H2_Db, 9mer_H2_Db, 8mer_H2_Db. Also study integrates prediction of peptide MHC class I binding; proteasomal C terminal cleavage and TAP transport efficiency by using sequence and properties of the amino acids. We also found the binding of peptides to different alleles by using Position Specific Scoring Matrix. Cytochrome B from Ascaris lumbricoides (365 residues long) with 357 nonamers having antigenic MHC binding peptides. PSSM based server will predict the peptide binders from sequence to MHCII molecules are as I_Ab.p, I_Ad.p, I_Ag7, which are found antigenic epitopes region in Cytochrome B from Ascaris lumbricoides. This investigation can be useful in rational vaccine design and simultaneously increase the understanding the role of the immune system against antigenic.
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