4.7 Article

Pre-clinical evaluation of a whole-parasite vaccine to control human babesiosis

Journal

CELL HOST & MICROBE
Volume 29, Issue 6, Pages 894-+

Publisher

CELL PRESS
DOI: 10.1016/j.chom.2021.04.008

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Funding

  1. National Health and Medical Research Council (Australia) Program grant [APP1132975]

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Researchers have developed a whole-parasite Babesia vaccine using chemically attenuated B. microti parasitized red blood cells and produced liposomes containing killed parasite material. The vaccine significantly reduces peak parasitemia following challenge.
Babesia spp. are tick-transmitted intra-erythrocytic protozoan parasites that infect humans and animals, causing a flu-like illness and hemolytic anemia. There is currently no human vaccine available. People most at risk of severe disease are the elderly, immunosuppressed, and asplenic individuals. B. microti and B. divergens are the predominant species affecting humans. Here, we present a whole-parasite Babesia vaccine. To establish proof-of-principle, we employed chemically attenuated B. microti parasitized red blood cells from infected mice. To aid clinical translation, we produced liposomes containing killed parasite material. Vaccination significantly reduces peak parasitemia following challenge. B cells and anti-parasite antibodies do not significantly contribute to vaccine efficacy. Protection is abrogated by the removal of CD4(+) T cells or macrophages prior to challenge. Importantly, splenectomized mice are protected by vaccination. To further facilitate translation, we prepared a culture-based liposomal vaccine and demonstrate that this performs as a universal vaccine inducing immunity against different human Babesia species.

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