Expression and characterization of genetically engineered human immunodeficiency virus-like particles containing modified envelope glycoproteins: implications for development of a cross-protective AIDS vaccine.

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J Virol. 1992 July; 66(7): 4003-4012

Expression and characterization of genetically engineered human immunodeficiency virus-like particles containing modified envelope glycoproteins: implications for development of a cross-protective AIDS vaccine.

B Rovinski, J R Haynes, S X Cao, O James, C Sia, S Zolla-Pazner, T J Matthews and M H Klein

Department of Molecular Genetics, Connaught Centre for Biotechnology Research, Willowdale, Ontario, Canada.

ABSTRACT

Noninfectious human immunodeficiency virus type 1 (HIV-1) viruslikeparticles containing chimeric envelope glycoproteins were expressedin mammalian cells by using inducible promoters. We engineeredfour expression vectors in which a synthetic oligomer encodinggp120 residues 306 to 328 (amino acids YNKRKRIHIGP GRAFYTTKNIIG)from the V3 loop of the MN viral isolate was inserted at variouspositions within the endogenous HIV-1LAI env gene. Expressionstudies revealed that insertion of the heterologous V3(MN) loopsegment at two different locations within the conserved region2 (C2) of gp120, either 173 or 242 residues away from the Nterminus of the mature subunit, resulted in the secretion offully assembled HIV-like particles containing chimeric LAI/MNenvelope glycoproteins. Both V3 loop epitopes were recognizedby loop-specific neutralizing antibodies. However, insertionof the V3(MN) loop segment into other regions of gp120 led tothe production of envelope-deficient viruslike particles. Immunizationwith HIV-like particles containing chimeric envelope proteinsinduced specific antibody responses against both the autologousand heterologous V3 loop epitopes, including cross-neutralizingantibodies against the HIV-1LAI and HIV-1MN isolates. This study,therefore, demonstrates the feasibility of genetically engineeringoptimized HIV-like particles capable of eliciting cross-neutralizingantibodies.

J Virol. 1992 July; 66(7): 4003-4012

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