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Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach

Hepatitis C is the major health problem over the globe affecting approximately 200 million people worldwide and about 10 million Pakistani populations. Developing countries are especially facing the problems of HCV infection. Hence the goal of the study was to find out the antigenic epitopes that co...

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Autores principales: Shehzadi, Abida, Rehman, Shahid Ur, Husnain, Tayyab
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Biomedical Informatics 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3524940/
https://www.ncbi.nlm.nih.gov/pubmed/23275687
http://dx.doi.org/10.6026/97320630008957
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author Shehzadi, Abida
Rehman, Shahid Ur
Husnain, Tayyab
author_facet Shehzadi, Abida
Rehman, Shahid Ur
Husnain, Tayyab
author_sort Shehzadi, Abida
collection PubMed
description Hepatitis C is the major health problem over the globe affecting approximately 200 million people worldwide and about 10 million Pakistani populations. Developing countries are especially facing the problems of HCV infection. Hence the goal of the study was to find out the antigenic epitopes that could be effective vaccine targets of HCV genotype 1 of Asian origin against HLA alleles frequently distributed in Asian countries. A total of 85 complete genome sequences of HCV 1 of Asian origin were retrieved from the HCV sequence database. Using in silico tools, T cell epitopes were predicted from conserved regions of all the available HCV 1 subtypes against Asian HLA alleles. Using 10 MHC I supertypes 51 epitopes was predicted as promiscuous binders. MHC class I supertypes A2 and B7 were found to be good promiscuous binders for a large number of predicted epitopes. Other alleles of MHC I supertypes (B57, B27, BX, B44) either were not respondent as promiscuous binders or responded only to a limited number of epitopes. Against 8 predominantly found Asian alleles of DRB1 supertype, 42 epitopes was predicted as promiscuous binders. MHC class II alleles DRB1-0101, DRB1-0701 and DRB1-1501 were the highest binders to promiscuous predicted epitopes while DRB1-0301 was the least binder for the predicted promiscuous epitopes of HCV 1 genotype of Asian origin. Literature review survey of predicted epitopes via IEDB also confirmed that great numbers of predicted epitopes are true positive. Hence, sophisticated selection of viral proteins and MHCs provided conserved promiscuous epitopes that can be used as effective vaccine candidates for all Asian counties. ABBREVIATIONS: HCV - hepatitis C virus, MHC - major histocompatability complex, HLA - human leukocyte antigen, CTL - cytotoxic T lymphocytes.
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spelling pubmed-35249402012-12-28 Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach Shehzadi, Abida Rehman, Shahid Ur Husnain, Tayyab Bioinformation Hypothesis Hepatitis C is the major health problem over the globe affecting approximately 200 million people worldwide and about 10 million Pakistani populations. Developing countries are especially facing the problems of HCV infection. Hence the goal of the study was to find out the antigenic epitopes that could be effective vaccine targets of HCV genotype 1 of Asian origin against HLA alleles frequently distributed in Asian countries. A total of 85 complete genome sequences of HCV 1 of Asian origin were retrieved from the HCV sequence database. Using in silico tools, T cell epitopes were predicted from conserved regions of all the available HCV 1 subtypes against Asian HLA alleles. Using 10 MHC I supertypes 51 epitopes was predicted as promiscuous binders. MHC class I supertypes A2 and B7 were found to be good promiscuous binders for a large number of predicted epitopes. Other alleles of MHC I supertypes (B57, B27, BX, B44) either were not respondent as promiscuous binders or responded only to a limited number of epitopes. Against 8 predominantly found Asian alleles of DRB1 supertype, 42 epitopes was predicted as promiscuous binders. MHC class II alleles DRB1-0101, DRB1-0701 and DRB1-1501 were the highest binders to promiscuous predicted epitopes while DRB1-0301 was the least binder for the predicted promiscuous epitopes of HCV 1 genotype of Asian origin. Literature review survey of predicted epitopes via IEDB also confirmed that great numbers of predicted epitopes are true positive. Hence, sophisticated selection of viral proteins and MHCs provided conserved promiscuous epitopes that can be used as effective vaccine candidates for all Asian counties. ABBREVIATIONS: HCV - hepatitis C virus, MHC - major histocompatability complex, HLA - human leukocyte antigen, CTL - cytotoxic T lymphocytes. Biomedical Informatics 2012-10-13 /pmc/articles/PMC3524940/ /pubmed/23275687 http://dx.doi.org/10.6026/97320630008957 Text en © 2012 Biomedical Informatics This is an open-access article, which permits unrestricted use, distribution, and reproduction in any medium, for non-commercial purposes, provided the original author and source are credited.
spellingShingle Hypothesis
Shehzadi, Abida
Rehman, Shahid Ur
Husnain, Tayyab
Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title_full Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title_fullStr Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title_full_unstemmed Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title_short Selection of epitope-based vaccine targets of HCV genotype 1 of Asian origin: a systematic in silico approach
title_sort selection of epitope-based vaccine targets of hcv genotype 1 of asian origin: a systematic in silico approach
topic Hypothesis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3524940/
https://www.ncbi.nlm.nih.gov/pubmed/23275687
http://dx.doi.org/10.6026/97320630008957
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