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

Hanan A. Al-Nazal; Emily Cooper; Mei Fong Ho; Sharareh Eskandari; Victoria Majam; Ashwini Kumar Giddam; Waleed M. Hussein; Md Tanjir Islam; Mariusz Skwarczynski; Istvan Toth; Sanjai Kumar; Ali Zaid; Michael Batzloff; Danielle I. Stanisic; Michael F. Good

doi:10.1016/j.chom.2021.04.008

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

Hanan A. Al-Nazal, Emily Cooper, Mei Fong Ho, Sharareh Eskandari, Victoria Majam, Ashwini Kumar Giddam, Waleed M. Hussein, Md Tanjir Islam, Mariusz Skwarczynski, Istvan Toth, Sanjai Kumar, Ali Zaid, Michael Batzloff, Danielle I. Stanisic, Michael F. Good

Research output: Contribution to journal › Article › Research › peer-review

21 Citations (Scopus)

Abstract

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.

Original language	English
Pages (from-to)	894-903
Number of pages	10
Journal	Cell Host & Microbe
Volume	29
Issue number	6
DOIs	https://doi.org/10.1016/j.chom.2021.04.008
Publication status	Published - 9 Jun 2021
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

B. divergens
B. microti
Babesia
heterologous protection
immunity
T cells
vaccine
whole parasite vaccine

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10.1016/j.chom.2021.04.008

Cite this

Al-Nazal, H. A., Cooper, E., Ho, M. F., Eskandari, S., Majam, V., Giddam, A. K., Hussein, W. M., Islam, M. T., Skwarczynski, M., Toth, I., Kumar, S., Zaid, A., Batzloff, M., Stanisic, D. I., & Good, M. F. (2021). Pre-clinical evaluation of a whole-parasite vaccine to control human babesiosis. Cell Host & Microbe, 29(6), 894-903. https://doi.org/10.1016/j.chom.2021.04.008

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abstract = "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.",

keywords = "B. divergens, B. microti, Babesia, heterologous protection, immunity, T cells, vaccine, whole parasite vaccine",

author = "Al-Nazal, \{Hanan A.\} and Emily Cooper and Ho, \{Mei Fong\} and Sharareh Eskandari and Victoria Majam and Giddam, \{Ashwini Kumar\} and Hussein, \{Waleed M.\} and Islam, \{Md Tanjir\} and Mariusz Skwarczynski and Istvan Toth and Sanjai Kumar and Ali Zaid and Michael Batzloff and Stanisic, \{Danielle I.\} and Good, \{Michael F.\}",

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doi = "10.1016/j.chom.2021.04.008",

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AU - Al-Nazal, Hanan A.

AU - Cooper, Emily

AU - Ho, Mei Fong

AU - Eskandari, Sharareh

AU - Majam, Victoria

AU - Giddam, Ashwini Kumar

AU - Hussein, Waleed M.

AU - Islam, Md Tanjir

AU - Skwarczynski, Mariusz

AU - Toth, Istvan

AU - Kumar, Sanjai

AU - Zaid, Ali

AU - Batzloff, Michael

AU - Stanisic, Danielle I.

AU - Good, Michael F.

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N2 - 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.

AB - 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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KW - B. microti

KW - Babesia

KW - heterologous protection

KW - immunity

KW - T cells

KW - vaccine

KW - whole parasite vaccine

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M3 - Article

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ER -

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

Abstract

UN SDGs

Keywords

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