Intranasal vaccination with lipid-conjugated immunogens promotes antigen transmucosal uptake to drive mucosal and systemic immunity

Author:

Hartwell Brittany L.12ORCID,Melo Mariane B.123ORCID,Xiao Peng4ORCID,Lemnios Ashley A.1,Li Na1,Chang Jason Y.H.12ORCID,Yu Jingyou5ORCID,Gebre Makda S.5ORCID,Chang Aiquan56ORCID,Maiorino Laura1ORCID,Carter Crystal4ORCID,Moyer Tyson J.123,Dalvie Neil C.17ORCID,Rodriguez-Aponte Sergio A.18ORCID,Rodrigues Kristen A.1239ORCID,Silva Murillo13ORCID,Suh Heikyung1,Adams Josetta1ORCID,Fontenot Jane4ORCID,Love J. Christopher17ORCID,Barouch Dan H.5ORCID,Villinger Francois410ORCID,Ruprecht Ruth M.4,Irvine Darrell J.123811ORCID

Affiliation:

1. Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

2. Ragon Institute of Massachusetts General Hospital, Massachusetts Institute of Technology and Harvard University, Cambridge, MA 02139, USA.

3. Consortium for HIV/AIDS Vaccine Development (CHAVD), Scripps Research Institute, La Jolla, CA 92037, USA.

4. New Iberia Research Center, University of Louisiana at Lafayette, New Iberia, LA 70560, USA.

5. Center for Virology and Vaccine Research, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02115, USA.

6. Harvard Medical School, Boston, MA 02115, USA.

7. Department of Chemical Engineering, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

8. Department of Biological Engineering, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

9. Harvard-MIT Health Sciences and Technology, Institute for Medical Engineering and Science, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

10. Department of Biology, University of Louisiana at Lafayette, New Iberia, LA 70560 USA.

11. Department of Materials Science and Engineering, Massachusetts Institute of Technology, Cambridge, MA 02139 USA.

Abstract

To combat the HIV epidemic and emerging threats such as SARS-CoV-2, immunization strategies are needed that elicit protection at mucosal portals of pathogen entry. Immunization directly through airway surfaces is effective in driving mucosal immunity, but poor vaccine uptake across the mucus and epithelial lining is a limitation. The major blood protein albumin is constitutively transcytosed bidirectionally across the airway epithelium through interactions with neonatal Fc receptors (FcRn). Exploiting this biology, here, we demonstrate a strategy of “albumin hitchhiking” to promote mucosal immunity using an intranasal vaccine consisting of protein immunogens modified with an amphiphilic albumin-binding polymer-lipid tail, forming amph-proteins. Amph-proteins persisted in the nasal mucosa of mice and nonhuman primates and exhibited increased uptake into the tissue in an FcRn-dependent manner, leading to enhanced germinal center responses in nasal-associated lymphoid tissue. Intranasal immunization with amph-conjugated HIV Env gp120 or SARS-CoV-2 receptor binding domain (RBD) proteins elicited 100- to 1000-fold higher antigen-specific IgG and IgA titers in the serum, upper and lower respiratory mucosa, and distal genitourinary mucosae of mice compared to unmodified protein. Amph-RBD immunization induced high titers of SARS-CoV-2–neutralizing antibodies in serum, nasal washes, and bronchoalveolar lavage. Furthermore, intranasal amph-protein immunization in rhesus macaques elicited 10-fold higher antigen-specific IgG and IgA responses in the serum and nasal mucosa compared to unmodified protein, supporting the translational potential of this approach. These results suggest that using amph-protein vaccines to deliver antigen across mucosal epithelia is a promising strategy to promote mucosal immunity against HIV, SARS-CoV-2, and other infectious diseases.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

General Medicine

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