Recognition of prominent viral epitopes induced by immunization with human immunodeficiency virus type 1 regulatory genes

Author:

Hinkula J1,Svanholm C1,Schwartz S1,Lundholm P1,Brytting M1,Engström G1,Benthin R1,Glaser H1,Sutter G1,Kohleisen B1,Erfle V1,Okuda K1,Wigzell H1,Wahren B1

Affiliation:

1. Microbiology and Tumorbiology Center, Karolinska Institute, Stockholm, Sweden. Jorma.Hinkula@smi.ki.se

Abstract

Mice immunized with the regulatory genes nef, rev, and tat from human immunodeficiency virus type 1 developed both humoral and cellular immune responses to the gene products Nef, Rev, and Tat. This study demonstrates that it is feasible to induce immune reactions to all of these regulatory gene products. Humoral responses were seen after DNA boosts, while potent T-cell proliferative responses were noted already after a single immunization. A Th1-directed immune response was demonstrated early after immunization. A 3- to 75-fold-stronger T-cell response was seen in animals receiving DNA epidermally compared to that in animals receiving intramuscular injections. Nef, Rev, and Tat putative B- and T-cell epitopes were clearly mapped by using peptides derived from the regulatory proteins and were similar to those which are detected in human immunodeficiency virus infection. Although immunization by the Nef, Rev, and Tat proteins raised high immunoglobulin G titers in serum, the epitope spreading appeared broader after DNA immunization. The combination of all of these regulatory genes together with two genes for structural proteins, the envelope and gag genes, demonstrated that a combined approach is feasible in that reactivities to all antigens persisted or were even augmented. No interference between plasmids was noted.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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