Plasmodium berghei Brca2 is required for normal development and differentiation in mice and mosquitoes

Yasunaga Yoshikawa; Shunta Kimura; Akira Soga; Makoto Sugiyama; Aki Ueno; Hiroki Kondo; Zida Zhu; Kazuhiko Ochiai; Kazuhiko Nakayama; Jun Hakozaki; Kodai Kusakisako; Asako Haraguchi; Taisuke Kitano; Koichi Orino; Shinya Fukumoto; Hiromi Ikadai

doi:10.1186/s13071-022-05357-w

Plasmodium berghei Brca2 is required for normal development and differentiation in mice and mosquitoes

Parasit Vectors. 2022 Jul 8;15(1):244. doi: 10.1186/s13071-022-05357-w.

Authors

Affiliations

¹ Laboratory of Veterinary Biochemistry, School of Veterinary Medicine, Kitasato University, Towada, Aomori, 034-8628, Japan. yyoshika@vmas.kitasato-u.ac.jp.
² Laboratory of Veterinary Biochemistry, School of Veterinary Medicine, Kitasato University, Towada, Aomori, 034-8628, Japan.
³ National Research Center for Protozoan Diseases, Obihiro University of Agriculture and Veterinary Medicine, Inada, Obihiro, 080-8555, Japan.
⁴ Laboratory of Veterinary Anatomy, School of Veterinary Medicine, Kitasato University, Towada, Aomori, 034-8628, Japan.
⁵ Laboratory of Veterinary Hygiene, School of Veterinary Medicine, Nippon Veterinary and Life Science University, Musashino, Tokyo, 180-8602, Japan.
⁶ Laboratory of Veterinary Parasitology, School of Veterinary Medicine, Kitasato University, Towada, Aomori, 034-8628, Japan.

Abstract

Background: Malaria is a major global parasitic disease caused by species of the genus Plasmodium. Zygotes of Plasmodium spp. undergo meiosis and develop into tetraploid ookinetes, which differentiate into oocysts that undergo sporogony. Homologous recombination (HR) occurs during meiosis and introduces genetic variation. However, the mechanisms of HR in Plasmodium are unclear. In humans, the recombinases DNA repair protein Rad51 homolog 1 (Rad51) and DNA meiotic recombinase 1 (Dmc1) are required for HR and are regulated by breast cancer susceptibility protein 2 (BRCA2). Most eukaryotes harbor BRCA2 homologs. Nevertheless, these have not been reported for Plasmodium.

Methods: A Brca2 candidate was salvaged from a database to identify Brca2 homologs in Plasmodium. To confirm that the candidate protein was Brca2, interaction activity between Plasmodium berghei (Pb) Brca2 (PbBrca2) and Rad51 (PbRad51) was investigated using a mammalian two-hybrid assay. To elucidate the functions of PbBrca2, PbBrca2 was knocked out and parasite proliferation and differentiation were assessed in mice and mosquitoes. Transmission electron microscopy was used to identify sporogony.

Results: The candidate protein was conserved among Plasmodium species, and it was indicated that it harbors critical BRCA2 domains including BRC repeats, tower, and oligonucleotide/oligosaccharide-binding-fold domains. The P. berghei BRC repeats interacted with PbRad51. Hence, the candidate was considered a Brca2 homolog. PbBrca2 knockout parasites were associated with reduced parasitemia with increased ring stage and decreased trophozoite stage counts, gametocytemia, female gametocyte ratio, oocyst number, and ookinete development in both mice and mosquitoes. Nevertheless, the morphology of the blood stages in mice and the ookinete stage was comparable to those of the wild type parasites. Transmission electron microscopy results showed that sporogony never progressed in Brca2-knockout parasites.

Conclusions: Brca2 is implicated in nearly all Plasmodium life cycle stages, and especially in sporogony. PbBrca2 contributes to HR during meiosis.

Keywords: Breast cancer susceptibility protein 2; DNA repair protein Rad51 homolog 1; Homologous recombination; Meiosis; Plasmodium.

MeSH terms

Animals
Culicidae* / parasitology
Female
Homologous Recombination
Life Cycle Stages
Malaria*
Mammals
Mice
Oocysts / genetics
Parasites*
Plasmodium berghei / genetics

Abstract

MeSH terms

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