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Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens.

J Immunol.. 2016-04; 
Hessell AJ,Malherbe DC,Pissani F,McBurney S,Krebs SJ,Gomes M,Pandey S,Sutton WF,Burwitz BJ,Gray M,Robins H,Park BS,Sacha JB,LaBranche CC,Fuller DH,Montefiori DC,Stamatatos L,Sather DN,Haigwood NL.
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Peptide Synthesis ... The HIV-1 SF162 V3 peptide (PNNNTRKSITIGPGRAFYATGD), the MPER peptide (RRRNEQELLELDKWASLWNWFDITNWLWYIRRRR), and MPER scrambled peptide (KKKRIYWLWNTIDFWNWLSAWKDLELLEQENKKK) were synthesized by Genscript (Piscataway, ... Get A Quote

摘要

Advancement in immunogen selection and vaccine design that will rapidly elicit a protective Ab response is considered critical for HIV vaccine protective efficacy. Vaccine-elicited Ab responses must therefore have the capacity to prevent infection by neutralization-resistant phenotypes of transmitted/founder (T/F) viruses that establish infection in humans. Most vaccine candidates to date have been ineffective at generating Abs that neutralize T/F or early variants. In this study, we report that coimmunizing rhesus macaques with HIV-1 gp160 DNA and gp140 trimeric protein selected from native envelope gene sequences (envs) induced neutralizing Abs against Tier 2 autologous viruses expressing cognate envelope (En... More

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