Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment

The human papillomavirus (HPV) 9-valent, recombinant vaccine (Gardasil™9) helps protect young adults (males and females) against anogenital cancers and genital warts caused by certain HPV genotypes (ref. Gardasil™9 insert). This vaccine is administered intramuscularly (IM). The aim of this study was...

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Autores principales: Meyer, Brian K., Kendall, Mark A.F., Williams, Donna M., Bett, Andrew J., Dubey, Sheri, Gentzel, Renee C., Casimiro, Danilo, Forster, Angus, Corbett, Holly, Crichton, Michael, Baker, S. Ben, Evans, Robert K., Bhambhani, Akhilesh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Regular paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6668242/
https://www.ncbi.nlm.nih.gov/pubmed/31384745
http://dx.doi.org/10.1016/j.jvacx.2019.100030
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author Meyer, Brian K.
Kendall, Mark A.F.
Williams, Donna M.
Bett, Andrew J.
Dubey, Sheri
Gentzel, Renee C.
Casimiro, Danilo
Forster, Angus
Corbett, Holly
Crichton, Michael
Baker, S. Ben
Evans, Robert K.
Bhambhani, Akhilesh
author_facet Meyer, Brian K.
Kendall, Mark A.F.
Williams, Donna M.
Bett, Andrew J.
Dubey, Sheri
Gentzel, Renee C.
Casimiro, Danilo
Forster, Angus
Corbett, Holly
Crichton, Michael
Baker, S. Ben
Evans, Robert K.
Bhambhani, Akhilesh
author_sort Meyer, Brian K.
collection PubMed
description The human papillomavirus (HPV) 9-valent, recombinant vaccine (Gardasil™9) helps protect young adults (males and females) against anogenital cancers and genital warts caused by certain HPV genotypes (ref. Gardasil™9 insert). This vaccine is administered intramuscularly (IM). The aim of this study was to determine preclinically whether intradermal (ID) vaccination with an unadjuvanted 9-valent recombinant HPV vaccine using a first-generation ID delivery device, the Nanopatch™, could enhance vaccine immunogenicity compared with the traditional ID route (Mantoux technique). IM injection of HPV VLPs formulated with Merck & Co., Inc., Kenilworth, NJ, USA Alum Adjuvant (MAA) were included in the rhesus study for comparison. The Nanopatch™ prototype contains a high-density array comprised of 10,000 microprojections/cm(2), each 250 µm long. It was hypothesized the higher density array with shallower ID delivery may be superior to the Mantoux technique. To test this hypothesis, HPV VLPs without adjuvant were coated on the Nanopatch™, stability of the Nanopatch™ with unadjuvanted HPV VLPs were evaluated under accelerated conditions, skin delivery was verified using radiolabelled VLPs or FluoSpheres®, and the immune response and skin site reaction with the Nanopatch™ was evaluated in rhesus macaques. The immune response induced by Nanopatch™ administration, measured as HPV-specific binding antibodies, was similar to that induced using the Mantoux technique. It was also observed that a lower dose of unadjuvanted HPV VLPs delivered with the first-generation Nanopatch™ and applicator or Mantoux technique resulted in an immune response that was significantly lower compared to a higher-dose of alum adjuvanted HPV VLPs delivered IM in rhesus macaques. The study also indicated unadjuvanted HPV VLPs could be delivered with the first-generation Nanopatch™ and applicator to the skin in 15 s with a transfer efficiency of approximately 20%. This study is the first demonstration of patch administration in non-human primates with a vaccine composed of HPV VLPs.
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spelling pubmed-66682422019-08-05 Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment Meyer, Brian K. Kendall, Mark A.F. Williams, Donna M. Bett, Andrew J. Dubey, Sheri Gentzel, Renee C. Casimiro, Danilo Forster, Angus Corbett, Holly Crichton, Michael Baker, S. Ben Evans, Robert K. Bhambhani, Akhilesh Vaccine X Regular paper The human papillomavirus (HPV) 9-valent, recombinant vaccine (Gardasil™9) helps protect young adults (males and females) against anogenital cancers and genital warts caused by certain HPV genotypes (ref. Gardasil™9 insert). This vaccine is administered intramuscularly (IM). The aim of this study was to determine preclinically whether intradermal (ID) vaccination with an unadjuvanted 9-valent recombinant HPV vaccine using a first-generation ID delivery device, the Nanopatch™, could enhance vaccine immunogenicity compared with the traditional ID route (Mantoux technique). IM injection of HPV VLPs formulated with Merck & Co., Inc., Kenilworth, NJ, USA Alum Adjuvant (MAA) were included in the rhesus study for comparison. The Nanopatch™ prototype contains a high-density array comprised of 10,000 microprojections/cm(2), each 250 µm long. It was hypothesized the higher density array with shallower ID delivery may be superior to the Mantoux technique. To test this hypothesis, HPV VLPs without adjuvant were coated on the Nanopatch™, stability of the Nanopatch™ with unadjuvanted HPV VLPs were evaluated under accelerated conditions, skin delivery was verified using radiolabelled VLPs or FluoSpheres®, and the immune response and skin site reaction with the Nanopatch™ was evaluated in rhesus macaques. The immune response induced by Nanopatch™ administration, measured as HPV-specific binding antibodies, was similar to that induced using the Mantoux technique. It was also observed that a lower dose of unadjuvanted HPV VLPs delivered with the first-generation Nanopatch™ and applicator or Mantoux technique resulted in an immune response that was significantly lower compared to a higher-dose of alum adjuvanted HPV VLPs delivered IM in rhesus macaques. The study also indicated unadjuvanted HPV VLPs could be delivered with the first-generation Nanopatch™ and applicator to the skin in 15 s with a transfer efficiency of approximately 20%. This study is the first demonstration of patch administration in non-human primates with a vaccine composed of HPV VLPs. Elsevier 2019-06-20 /pmc/articles/PMC6668242/ /pubmed/31384745 http://dx.doi.org/10.1016/j.jvacx.2019.100030 Text en © 2019 Merck Sharp & Dohme & Corp. and the Authors. http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Regular paper
Meyer, Brian K.
Kendall, Mark A.F.
Williams, Donna M.
Bett, Andrew J.
Dubey, Sheri
Gentzel, Renee C.
Casimiro, Danilo
Forster, Angus
Corbett, Holly
Crichton, Michael
Baker, S. Ben
Evans, Robert K.
Bhambhani, Akhilesh
Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title_full Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title_fullStr Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title_full_unstemmed Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title_short Immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation Nanopatch™ in rhesus macaques: An exploratory, pre-clinical feasibility assessment
title_sort immune response and reactogenicity of an unadjuvanted intradermally delivered human papillomavirus vaccine using a first generation nanopatch™ in rhesus macaques: an exploratory, pre-clinical feasibility assessment
topic Regular paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6668242/
https://www.ncbi.nlm.nih.gov/pubmed/31384745
http://dx.doi.org/10.1016/j.jvacx.2019.100030
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