Co-immunization of DNA and Protein in the Same Anatomical Sites Induces Superior Protective Immune Responses against SHIV Challenge

在同一解剖部位同时接种DNA和蛋白质可诱导针对SHIV攻击的更强效的保护性免疫反应

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作者:Barbara K Felber ,Zhongyan Lu ,Xintao Hu ,Antonio Valentin ,Margherita Rosati ,Christopher A L Remmel ,Joshua A Weiner ,Margaret C Carpenter ,Katelyn Faircloth ,Sherry Stanfield-Oakley ,Wilton B Williams ,Xiaoying Shen ,Georgia D Tomaras ,Celia C LaBranche ,David Montefiori ,Hung V Trinh ,Mangala Rao ,Munir S Alam ,Nathan A Vandergrift ,Kevin O Saunders ,Yunfei Wang ,Wes Rountree ,Jishnu Das ,Galit Alter ,Steven G Reed ,Pyone P Aye ,Faith Schiro ,Bapi Pahar ,Jason P Dufour ,Ronald S Veazey ,Preston A Marx ,David J Venzon ,George M Shaw ,Guido Ferrari ,Margaret E Ackerman ,Barton F Haynes ,George N Pavlakis

Abstract

We compare immunogenicity and protective efficacy of an HIV vaccine comprised of env and gag DNA and Env (Envelope) proteins by co-administration of the vaccine components in the same muscles or by separate administration of DNA + protein in contralateral sites in female rhesus macaques. The 6-valent vaccine includes gp145 Env DNAs, representing six sequentially isolated Envs from the HIV-infected individual CH505, and matching GLA-SE-adjuvanted gp120 Env proteins. Interestingly, only macaques in the co-administration vaccine group are protected against SHIV CH505 acquisition after repeated low-dose intravaginal challenge and show 67% risk reduction per exposure. Macaques in the co-administration group develop higher Env-specific humoral and cellular immune responses. Non-neutralizing Env antibodies, ADCC, and antibodies binding to FcγRIIIa are associated with decreased transmission risk. These data suggest that simultaneous recognition, processing, and presentation of DNA + Env protein in the same draining lymph nodes play a critical role in the development of protective immunity.

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