Author: Karch, Christopher P; Matyas, Gary R; Burkhard, Peter; Beck, Zoltan
Title: Glycosylation of the HIV-1 Env V1V2 loop to form a native-like structure may not be essential with a nanoparticle vaccine Document date: 2019_1_10
ID: yhh3ydok_4
Snippet: One of the most important regions of the HIV-1 Env protein is the V1V2 loop. IgG antibodies raised against this loop were inversely correlated with the risk of infection in the RV144 clinical trial [29] . Studies indicate that the V1V2 loop of the protein does not assume a unique defined structure [30] . As a result of the high density of glycans on the Env protein, most efforts in subunit vaccine development have used mammalian cells for bio-pro.....
Document: One of the most important regions of the HIV-1 Env protein is the V1V2 loop. IgG antibodies raised against this loop were inversely correlated with the risk of infection in the RV144 clinical trial [29] . Studies indicate that the V1V2 loop of the protein does not assume a unique defined structure [30] . As a result of the high density of glycans on the Env protein, most efforts in subunit vaccine development have used mammalian cells for bio-production. However, similar to the influenza hemagglutinin, a potential HIV-1 V1V2 vaccine candidate could be developed with an antigen that is expressed in E. coli, without glycosylation but with native-like conformation to induce high titers of high affinity antibodies that could prevent the initial infection [31] .
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