Protective Efficacy and Long-Term Immunogenicity in Cynomolgus Macaques by Ebola Virus Glycoprotein Synthetic DNA Vaccines

Author:

Patel Ami1,Reuschel Emma L1,Kraynyak Kimberly A2,Racine Trina34,Park Daniel H1,Scott Veronica L5,Audet Jonathan34,Amante Dinah2,Wise Megan C2,Keaton Amelia A1,Wong Gary3,Villarreal Daniel O6,Walters Jewell2,Muthumani Kar1,Shedlock Devon J6,de La Vega Marc-Antoine3,Plyler Ross6,Boyer Jean2,Broderick Kate E2,Yan Jian2,Khan Amir S2,Jones Shane3,Bello Alexander3,Soule Geoff3,Tran Kaylie N3,He Shihua3,Tierney Kevin3,Qiu Xiangguo34,Kobinger Gary P67,Sardesai Niranjan Y2,Weiner David B1

Affiliation:

1. The Wistar Institute of Anatomy and Biology, Philadelphia, Pennsylvania

2. Inovio Pharmaceuticals Inc., Plymouth Meeting, Pennsylvania

3. Special Pathogens Program, National Microbiology Laboratory, Public Health Agency of Canada, Winnipeg, Manitoba, Canada

4. Department of Medical Microbiology, University of Manitoba, Winnipeg, Canada

5. College of Osteopathic Medicine, William Carey University, Hattiesburg, Mississippi

6. University of Pennsylvania, Philadelphia

7. Université Laval, Québec, Canada

Abstract

Abstract Background There remains an important need for prophylactic anti-Ebola virus vaccine candidates that elicit long-lasting immune responses and can be delivered to vulnerable populations that are unable to receive live-attenuated or viral vector vaccines. Methods We designed novel synthetic anti-Ebola virus glycoprotein (EBOV-GP) DNA vaccines as a strategy to expand protective breadth against diverse EBOV strains and evaluated the impact of vaccine dosing and route of administration on protection against lethal EBOV-Makona challenge in cynomolgus macaques. Long-term immunogenicity was monitored in nonhuman primates for >1 year, followed by a 12-month boost. Results Multiple-injection regimens of the EBOV-GP DNA vaccine, delivered by intramuscular administration followed by electroporation, were 100% protective against lethal EBOV-Makona challenge. Impressively, 2 injections of a simple, more tolerable, and dose-sparing intradermal administration followed by electroporation generated strong immunogenicity and was 100% protective against lethal challenge. In parallel, we observed that EBOV-GP DNA vaccination induced long-term immune responses in macaques that were detectable for at least 1 year after final vaccination and generated a strong recall response after the final boost. Conclusions These data support that this simple intradermal-administered, serology-independent approach is likely important for additional study towards the goal of induction of anti-EBOV immunity in multiple at-risk populations.

Funder

Defense Advanced Research Projects Agency

Inovio Pharmaceuticals

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Immunology and Allergy

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