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      Intranasal Nanoemulsion-Adjuvanted HSV-2 Subunit Vaccine is Effective as a Prophylactic and Therapeutic Vaccine Using the Guinea Pig Model of Genital Herpes

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          Abstract

          Genital herpes is a sexually transmitted disease representing a major global health concern. Currently, there is no approved vaccine and existing antiviral therapies exhibit limited efficacy. Herein, we describe an intranasal (IN) vaccine comprised of HSV-2 surface glycoproteins gD2 and gB2 formulated in a nanoemulsion adjuvant (NE01-gD2/gB2). Using the HSV-2 genital herpes guinea pig model, we demonstrate that IN NE01-gD2/gB2 induces higher levels of neutralizing antibody compared to a monovalent IN NE01-gD2 vaccine, but less than an intramuscular (IM) Alum/MPL-gD2 vaccine. Following intravaginal (IVag) challenge with HSV-2, the group immunized with IN NE01-gD2/gB2 exhibited significantly reduced acute and recurrent disease scores compared to placebo recipients. Significantly, latent virus was only detected in the dorsal root ganglia of 1 of 12 IN NE01-gD2/gB2-vaccinated animals compared to 11 of 12 placebo recipient. In the therapeutic model, IN NE01-gD2/gB2 immunized guinea pigs exhibited a significant reduction in the recurrent lesions scores (64%, p<0.01), number of animal days with disease (64%, p<0.01), number of animals with viral shedding (50%, p<0.04) and reduction in virus positive vaginal swabs (56%, p<0.04), These data suggests that the treatment may be effective in treating chronic disease and minimizing virus transmission. These results warrant advancing the development of IN NE01-gD2/gB2 as both a prophylactic and therapeutic vaccine against HSV-2.

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          Author and article information

          Journal
          8406899
          7945
          Vaccine
          Vaccine
          Vaccine
          0264-410X
          1873-2518
          12 September 2019
          09 September 2019
          08 October 2019
          08 October 2020
          : 37
          : 43
          : 6470-6477
          Affiliations
          [a ]Cincinnati Children’s Hospital Medical Center, Cincinnati, OH, USA
          [b ]BlueWillow Biologics, Ann Arbor MI, USA
          [c ]University of Pennsylvania, Philadelphia, PA, USA
          Author notes
          [* ]Corresponding authors: David Bernstein, MD, Cincinnati Children Hospital Medical Center, 3333 Burnet Ave, Cincinnati, Ohio 45229, USA, david.bernstein@ 123456cchmc.org ; Ali Fattom, PhD, 2311 Green Road, Suite A, Ann Arbor, MI 48105, USA, ali.fattom@ 123456bluewillow.com

          Author contributions: DB, RC, TH, VB and AF, contributed to concept, protocol designs, data analysis and interpretation, FB and DPexecuted the animal work and data collection. GC provided the antigens and participated in interpretation of data. DB, RC, TH and AF contributed to the writing of the manuscript and approved the final version of the manuscript.

          Article
          PMC7017967 PMC7017967 7017967 nihpa1539464
          10.1016/j.vaccine.2019.08.077
          7017967
          31515143
          7b97074c-bb2d-42e2-a531-834b0841d93c
          History
          Categories
          Article

          NanoVax,nanoemulsion,herpes simplex virus type 2,genital herpes,vaccine

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