The Cross-Species Immunity During Acute Babesia Co-Infection in Mice

Iqra Zafar; Eloiza May Galon; Daisuke Kondoh; Artemis Efstratiou; Jixu Li; Shengwei Ji; Mingming Liu; Yongchang Li; Yae Hasegawa; Jinlin Zhou; Xuenan Xuan

doi:10.3389/fcimb.2022.885985

The Cross-Species Immunity During Acute Babesia Co-Infection in Mice

Front Cell Infect Microbiol. 2022 May 27:12:885985. doi: 10.3389/fcimb.2022.885985. eCollection 2022.

Authors

Iqra Zafar^{1

2}, Eloiza May Galon¹, Daisuke Kondoh³, Artemis Efstratiou⁴, Jixu Li^{1

5}, Shengwei Ji¹, Mingming Liu^{1

6}, Yongchang Li^{1

7}, Yae Hasegawa¹, Jinlin Zhou⁸, Xuenan Xuan¹

Affiliations

¹ National Research Center for Protozoan Diseases, Obihiro University of Agriculture and Veterinary Medicine, Obihiro, Japan.
² Livestock and Dairy Development Department, Veterinary Research Institute, Lahore, Pakistan.
³ Department of Veterinary Medicine, Obihiro University of Agriculture and Veterinary Medicine, Obihiro, Japan.
⁴ Max Planck Institute for Evolutionary Biology, Plön, Germany.
⁵ College of Agriculture and Animal Husbandry, Qinghai University, Xining, China.
⁶ Department of Microbiology and Immunology, School of Basic Medicine, Hubei University of Arts and Science, Xiangyang, China.
⁷ Parasitology Laboratory, Veterinary College, Xinjiang Agricultural University, Urumqi, China.
⁸ Shanghai Veterinary Research Institute, Chinese Academy of Agricultural Sciences, Shanghai, China.

Abstract

Babesiosis causes high morbidity and mortality in immunocompromised individuals. An earlier study suggested that lethal Babesia rodhaini infection in murine can be evaded by Babesia microti primary infection via activated macrophage-based immune response during the chronic stage of infection. However, whether the same immune dynamics occur during acute B. microti co-infection is not known. Hence, we used the mouse model to investigate the host immunity during simultaneous acute disease caused by two Babesia species of different pathogenicity. Results showed that B. microti primary infection attenuated parasitemia and conferred immunity in challenge-infected mice as early as day 4 post-primary infection. Likewise, acute Babesia co-infection undermined the splenic immune response, characterized by the significant decrease in splenic B and T cells leading to the reduction in antibody levels and decline in humoral immunity. Interestingly, increased macrophage and natural killer splenic cell populations were observed, depicting their subtle role in the protection. Pro-inflammatory cytokines (i.e. IFN-γ, TNF-α) were downregulated, while the anti-inflammatory cytokine IL-10 was upregulated in mouse sera during the acute phase of Babesia co-infection. Herein, the major cytokines implicated in the lethality caused by B. rodhaini infection were IFN- γ and IL-10. Surprisingly, significant differences in the levels of serum IFN- γ and IL-10 between co-infected survival groups (day 4 and 6 challenge) indicated that even a two-day delay in challenge infection was crucial for the resulting pathology. Additionally, oxidative stress in the form of reactive oxygen species contributed to the severity of pathology during acute babesiosis. Histopathological examination of the spleen showed that the erosion of the marginal zone was more pronounced during B. rodhaini infection, while the loss of cellularity of the marginal zone was less evident during co-infection. Future research warrants investigation of the roles of various immune cell subtypes in the mechanism involved in the protection of Babesia co-infected hosts.

Keywords: Babesia microti; Babesia rodhaini; acute stage; babesiosis; co-infection; innate immunity; oxidative stress; tick-borne infection.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Babesia*
Babesiosis*
Coinfection*
Cytokines
Infections*
Interferon-gamma
Interleukin-10
Mice
Mice, Inbred BALB C

Substances

Cytokines
Interleukin-10
Interferon-gamma