Development and Testing of a Spray-Dried Tuberculosis Vaccine Candidate in a Mouse Model

Mellissa Gomez; Mushtaq Ahmed; Shibali Das; Joseph McCollum; Leah Mellett; Rosemary Swanson; Ananya Gupta; Nicholas B Carrigy; Hui Wang; David Barona; Shital Bachchhav; Alana Gerhardt; Chris Press; Michelle C Archer; Hong Liang; Emilie Seydoux; Ryan M Kramer; Philip J Kuehl; Reinhard Vehring; Shabaana A Khader; Christopher B Fox

doi:10.3389/fphar.2021.799034

Development and Testing of a Spray-Dried Tuberculosis Vaccine Candidate in a Mouse Model

Front Pharmacol. 2022 Jan 21:12:799034. doi: 10.3389/fphar.2021.799034. eCollection 2021.

Authors

Mellissa Gomez¹, Mushtaq Ahmed², Shibali Das², Joseph McCollum³, Leah Mellett², Rosemary Swanson², Ananya Gupta², Nicholas B Carrigy¹, Hui Wang¹, David Barona¹, Shital Bachchhav¹, Alana Gerhardt³, Chris Press³, Michelle C Archer³, Hong Liang³, Emilie Seydoux³, Ryan M Kramer³, Philip J Kuehl⁴, Reinhard Vehring¹, Shabaana A Khader², Christopher B Fox^{3

5}

Affiliations

¹ Department of Mechanical Engineering, University of Alberta, Edmonton, AB, Canada.
² Department of Molecular Microbiology, Washington University in St. Louis, School of Medicine, St. Louis, MO, United States.
³ Infectious Disease Research Institute, Seattle, WA, United States.
⁴ Lovelace Biomedical, Albuquerque, NM, United States.
⁵ Department of Global Health, University of Washington, Seattle, WA, United States.

Abstract

Converting a vaccine into a thermostable dry powder is advantageous as it reduces the resource burden linked with the cold chain and provides flexibility in dosage and administration through different routes. Such a dry powder presentation may be especially useful in the development of a vaccine towards the respiratory infectious disease tuberculosis (TB). This study assesses the immunogenicity and protective efficacy of spray-dried ID93+GLA-SE, a promising TB vaccine candidate, against Mycobacterium tuberculosis (Mtb) in a murine model when administered via different routes. Four administration routes for the spray-dried ID93+GLA-SE were evaluated along with relevant controls-1) reconstitution and intramuscular injection, 2) reconstitution and intranasal delivery, 3) nasal dry powder delivery via inhalation, and 4) pulmonary dry powder delivery via inhalation. Dry powder intranasal and pulmonary delivery was achieved using a custom nose-only inhalation device, and optimization using representative vaccine-free powder demonstrated that approximately 10 and 44% of the maximum possible delivered dose would be delivered for intranasal delivery and pulmonary delivery, respectively. Spray-dried powder was engineered according to the different administration routes including maintaining approximately equivalent delivered doses of ID93 and GLA. Vaccine properties of the different spray-dried lots were assessed for quality control in terms of nanoemulsion droplet diameter, polydispersity index, adjuvant content, and antigen content. Our results using the Mtb mouse challenge model show that both intranasal reconstituted vaccine delivery as well as pulmonary dry powder vaccine delivery resulted in Mtb control in infected mice comparable to traditional intramuscular delivery. Improved protection in these two vaccinated groups over their respective control groups coincided with the presence of cytokine-producing T cell responses. In summary, our results provide novel vaccine formulations and delivery routes that can be harnessed to provide protection against Mtb infection.

Keywords: ID93+GLA-SE; dry powder vaccine; in vivo murine model; nose-only inhalation device; particle engineering; respiratory delivery; tuberculosis; vaccine adjuvant formulation.

Grants and funding

T32 HL007317/HL/NHLBI NIH HHS/United States