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Vol 50(2016) N 3 p. 353-361; DOI 10.1134/S0026893316030110 Full Text

A.N. Vzorov1,2*, R.W. Compans1

VLP vaccines and effects of HIV-1 Env protein modifications on their antigenic properties

1Department of Microbiology and Immunology and Emory Vaccine Center, Emory University School of Medicine, Atlanta, GA, 30322, USA
2Ivanovskii Institute of Virology, Gamaleya Federal Research Center for Epidemiology and Microbiology, Ministry of Healthcare of the Russian Federation, Moscow, 123098, Russia

*avzorov@emory.edu
Received - 2015-09-29; Accepted - 2015-11-23

An ideal protective HIV-1 vaccine can elicit broadly neutralizing antibodies, capable of preventing HIV transmission. The strategies of designing vaccines include generation of soluble recombinant proteins which mimic the native Env complex and are able to enhance the immunogenicity of gp120. Recent data indicate that the cytoplasmic tail (CT) of the Env protein has multiple functions, which can affect the early steps of infection, as well as viral assembly and antigenic properties. Modifications in the CT can be used to induce conformational changes in functional regions of gp120 and to stabilize the trimeric structure, avoiding immune misdirection and induction of non-neutralizing antibody responses. Env-trimers with modified CTs in virus-like particles (VLPs) are able to induce antibodies with broad spectrum neutralizing activity and high avidity and have the potential for developing an effective vaccine against HIV.

virus-like particles, HIV-1 vaccine, immunogen design, Env, envelope glycoproteins, cytoplasmic tail



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