The multiple stages of the malaria parasite life cycle hampers vaccine development. Combining a pre-erythrocytic antigen with a transmission-blocking antigen would target two independent stages of the life cycle for disease control, resulting in a multistage vaccine that can prevent infection and disease transmission simultaneously. Here, we generated a self-assembled ferritin nanoparticle vaccine that simultaneously presents designed immunogens CSPj5c and 17-4 from the infection-blocking circumsporozoite and the transmission-blocking Pfs48/45 antigens. These immunogens were designed, through structure-based approaches, to retain protective epitopes and confer protection upon vaccination. Immunization with CSPj5c-17-4-ferritin nanoparticles conferred protection against challenge with transgenic sporozoites expressing Plasmodium falciparum CSP in mice, and purified IgGs from immunized rabbits elicited potent transmission-reducing activity. Addition of the engineered 17-4 improved the immune responses to CSPj5c and protection from sporozoite challenge. CSPj5c-17-4-ferritin is therefore a promising multistage malaria vaccine with a potential role in malaria control.
A combined designed CSP and Pfs48/45 infection and transmission blocking vaccine for malaria.
一种结合了CSP和Pfs48/45的疟疾感染和传播阻断技术的疫苗
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作者:Gupta Richi, Dickey Thayne H, Salinas Nichole D, Patel Palak N, Ma Rui, Shi Dashuang, Singleton Myesha, Ouahes Tarik, Pham Thao P, Miura Kazutoyo, Long Carole A, Lambert Lynn E, Tolia Niraj H
| 期刊: | NPJ Vaccines | 影响因子: | 6.500 |
| 时间: | 2025 | 起止号: | 2025 Sep 2; 10(1):208 |
| doi: | 10.1038/s41541-025-01262-2 | ||
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