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Characterization of immune responses induced by combined clade-A HIV-1 recombinant adenovectors in mice.

作者信息

Bayanolhagh Saeed, Alinezhad Mahtab, Kamali Koorosh, Foroughi Maryam, Khorram Khorshid Hamid Reza, Mohraz Minoo, Mahboudi Fereidoun, Pourfathollah Ali Akbar

机构信息

Department of Immunology, Faculty of Medical Sciences, Tarbiat Modares University, Tehran, Iran, e-mail:

出版信息

Iran J Immunol. 2010 Sep;7(3):162-76.

PMID:20876987
Abstract

BACKGROUND

Numerous evidences indicate that in some HIV-1 positive patients, the humoral and cellular immune responses are induced against HIV-1 proteins and this is inversely related to the progress of infection.

OBJECTIVE

The aim of this study was the evaluation of the Adenovectors containing HIV genes in induction of immune responses in mice.

METHODS

The HIV-1 genes including gag p24, rev, nef and exon-1 of tat were amplified from HIV-1 RNA (clade-A). The cDNA of each gene was cloned into a transfer vector. The transfer vector was then co-transformed into E. coli strain BJ5183 together with pAdenovector ∆E1/E3. The recombinant adenoviral construct was transfected into QBI-293A cells. Recombinant viruses were purified and titrated on 293 cell plates. Expression of transgenes was evaluated using western blotting. Then 10(12) viral particles were injected into 15 groups of 5 mice and all patterns of combination of these 4 HIV-1 genes were evaluated. After 2 weeks, humoral and cellular immune responses were evaluated using ELISA, cell proliferation and ELISpot (IL-2, IL-4 and IFN-γ) assays, consecutively.

RESULTS

It was demonstrated that each gene was expressed. The response targets were mostly toward Th1, though several Th2 responses were also observed. Single injection in our study induced a good cellular response but the humoral responses were not as strong as the cellular ones.

CONCLUSION

Considering and comparing all results and evaluating the various possible interactions revealed that simultaneous injection of tat and gag has enhanced the humoral and cellular responses.

摘要

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