Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity

Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity

Introduction : Designing an effective vaccine against human immunodeficiency virus (HIV)-1 is a global health priority . Multi-epitope vaccines offer several potential advantages that may be promising in case of mutable divergent pathogens such as HIV-1. Herein, a multiepitopic recombinant protein c...

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Main Authors: Samira Arabi, Mohammad Reza Aghasadeghi, Arash Memarnejadian, Fatemeh Kohram, Haniyeh Aghababa, Nima Khoramabadi, Morteza Taghizadeh, Zahra Shahosseini, Mehdi Mahdavi
Format: Article
Language:English
Published: Pasteur Institute of Iran 2014-08-01
Series:Vaccine Research
Subjects:
hiv-1 tat/pol/gag/env
multi-epitope
protein expression
immune response
Online Access:http://vacres.pasteur.ac.ir/article-1-27-en.html
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spelling doaj-4fdf9657f956402890941b1d4f3d84b82020-11-25T03:51:30ZengPasteur Institute of IranVaccine Research2383-28192423-49232014-08-01111015Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on ImmunoreactivitySamira Arabi0Mohammad Reza Aghasadeghi1Arash Memarnejadian2Fatemeh Kohram3Haniyeh Aghababa4Nima Khoramabadi5Morteza Taghizadeh6Zahra Shahosseini7Mehdi Mahdavi8 Department of Biology, Science and Research Branch, Islamic Azad University, Tehran, Iran Department of Hepatitis and AIDS, Pasteur Institute of Iran, Tehran, Iran Department of Hepatitis and AIDS, Pasteur Institute of Iran, Tehran, Iran Department of Biotechnology, Tehran Shargh Branch, Payam-e-Nour University, Tehran, Iran Department of Bacteriology, Faculty of Medical Sciences, Tarbiat Modares University Department of Bacteriology, Faculty of Medical Sciences, Tarbiat Modares University Department of Medical virology, Tehran University of Medical Science, Tehran, Iran Department of Immunology, Pasteur Institute of Iran, Tehran, Iran Department of Immunology, Pasteur Institute of Iran, Tehran, Iran Introduction : Designing an effective vaccine against human immunodeficiency virus (HIV)-1 is a global health priority . Multi-epitope vaccines offer several potential advantages that may be promising in case of mutable divergent pathogens such as HIV-1. Herein, a multiepitopic recombinant protein containing various HIV-1 antigens was expressed in E. coli cells and its immunogenicity in combination with different adjuvants was initially evaluated in BALB/c mouse. Methods: HIVtop4 sequence spanning the junction of six amino acid fragments (Gag158-186, Pol150-190, ENV296-323, ENV577-610, Tat1-20 and Tat44-61) was designed based on immunoinformatic analysis to reduce the creation of junctional epitopes, improve the cleavage of proteasome and avoid the local accumulation of hydrophobic regions. Synthesized nucleotide sequence corresponding to HIVtop4 was cloned into pET23a plasmid. Expression of pET-HIVtop4 plasmid was induced in BL21 (DE3) E. coli cells by addition of 1 mM IPTG during 3 h culture and the protein was purified by Ni-NTA column chromatography and further confirmed against anti-His antibody in western-blotting. Groups of BALB/c mice (n=6) were immunized three times with 2 weeks interval, subcutaneously with 10 m g of candidate vaccine adjuvanted in Complete Freund’s adjuvant , Montanide ISA70 and Alum with suitable control groups. Two weeks after last immunization lymphocyte proliferation was measured with Brdu, IL-4 and IFN- g cytokines with ELISA, total antibody and IgG1, IgG2a isotypes with indirect ELISA methods. Results: Results showed that Immunization with HIV-1 tat/pol/gag/env led to a significant increase in the proliferative responses of lymphocytes, IL-4 and IFN-γ cytokine production and humoral immune response in comparison with the control groups. Conclusion: In this study we concluded that Tat, Env, Pol, Gag with adjuvants (Montanide, Alum and CFA) has potentials as a candidate vaccine against the HIV-1 virus. Vac Res, 2014, 1 (1): 10-15http://vacres.pasteur.ac.ir/article-1-27-en.htmlhiv-1 tat/pol/gag/envmulti-epitopeprotein expressionimmune response
collection DOAJ
language English
format Article
sources DOAJ
author Samira Arabi
Mohammad Reza Aghasadeghi
Arash Memarnejadian
Fatemeh Kohram
Haniyeh Aghababa
Nima Khoramabadi
Morteza Taghizadeh
Zahra Shahosseini
Mehdi Mahdavi
spellingShingle Samira Arabi
Mohammad Reza Aghasadeghi
Arash Memarnejadian
Fatemeh Kohram
Haniyeh Aghababa
Nima Khoramabadi
Morteza Taghizadeh
Zahra Shahosseini
Mehdi Mahdavi
Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
Vaccine Research
hiv-1 tat/pol/gag/env
multi-epitope
protein expression
immune response
author_facet Samira Arabi
Mohammad Reza Aghasadeghi
Arash Memarnejadian
Fatemeh Kohram
Haniyeh Aghababa
Nima Khoramabadi
Morteza Taghizadeh
Zahra Shahosseini
Mehdi Mahdavi
author_sort Samira Arabi
title Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
title_short Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
title_full Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
title_fullStr Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
title_full_unstemmed Cloning, Expression and Purification of a Novel Multi-epitopic HIV-1 Vaccine Candidate: A Preliminary Study on Immunoreactivity
title_sort cloning, expression and purification of a novel multi-epitopic hiv-1 vaccine candidate: a preliminary study on immunoreactivity
publisher Pasteur Institute of Iran
series Vaccine Research
issn 2383-2819
2423-4923
publishDate 2014-08-01
description Introduction : Designing an effective vaccine against human immunodeficiency virus (HIV)-1 is a global health priority . Multi-epitope vaccines offer several potential advantages that may be promising in case of mutable divergent pathogens such as HIV-1. Herein, a multiepitopic recombinant protein containing various HIV-1 antigens was expressed in E. coli cells and its immunogenicity in combination with different adjuvants was initially evaluated in BALB/c mouse. Methods: HIVtop4 sequence spanning the junction of six amino acid fragments (Gag158-186, Pol150-190, ENV296-323, ENV577-610, Tat1-20 and Tat44-61) was designed based on immunoinformatic analysis to reduce the creation of junctional epitopes, improve the cleavage of proteasome and avoid the local accumulation of hydrophobic regions. Synthesized nucleotide sequence corresponding to HIVtop4 was cloned into pET23a plasmid. Expression of pET-HIVtop4 plasmid was induced in BL21 (DE3) E. coli cells by addition of 1 mM IPTG during 3 h culture and the protein was purified by Ni-NTA column chromatography and further confirmed against anti-His antibody in western-blotting. Groups of BALB/c mice (n=6) were immunized three times with 2 weeks interval, subcutaneously with 10 m g of candidate vaccine adjuvanted in Complete Freund’s adjuvant , Montanide ISA70 and Alum with suitable control groups. Two weeks after last immunization lymphocyte proliferation was measured with Brdu, IL-4 and IFN- g cytokines with ELISA, total antibody and IgG1, IgG2a isotypes with indirect ELISA methods. Results: Results showed that Immunization with HIV-1 tat/pol/gag/env led to a significant increase in the proliferative responses of lymphocytes, IL-4 and IFN-γ cytokine production and humoral immune response in comparison with the control groups. Conclusion: In this study we concluded that Tat, Env, Pol, Gag with adjuvants (Montanide, Alum and CFA) has potentials as a candidate vaccine against the HIV-1 virus. Vac Res, 2014, 1 (1): 10-15
topic hiv-1 tat/pol/gag/env
multi-epitope
protein expression
immune response
url http://vacres.pasteur.ac.ir/article-1-27-en.html
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