A subunit vaccine Ag85A-LpqH focusing on humoral immunity provides substantial protection against tuberculosis in mice

Lingyuan Zeng; You Zuo; Minghui Tang; Chengrui Lei; Huoming Li; Xiuling Ma; Jiahong Ji; Hao Li

doi:10.1016/j.isci.2024.111568

A subunit vaccine Ag85A-LpqH focusing on humoral immunity provides substantial protection against tuberculosis in mice

iScience. 2024 Dec 20;28(1):111568. doi: 10.1016/j.isci.2024.111568. eCollection 2025 Jan 17.

Authors

Lingyuan Zeng¹, You Zuo¹, Minghui Tang¹, Chengrui Lei¹, Huoming Li¹, Xiuling Ma¹, Jiahong Ji¹, Hao Li¹

Affiliation

¹ National Key Laboratory of Veterinary Public Health and Safety, College of Veterinary Medicine, China Agricultural University, Beijing, China.

Abstract

The importance of humoral immunity in combating TB has gained extensive recognition. In this study, a subunit vaccine named Ag85A-LpqH (AL) was prepared by fusing the antigen Ag85A proved to induce robust T cell immune responses, and LpqH was shown to produce protective antibodies. The prevention and BCG prime-boost mouse models were established to test the vaccine efficacy. The results indicate that Ag85A-LpqH can induce substantial protection by reducing bacterial loads and pathological lesions. This vaccine can induce robust antibody responses, as well as T cell immune responses especially strong CD8⁺ T cell responses. Moreover, the serum from AL-immunized mice can reduce the bacterial load and lung pathology in mice. B cell receptor (BCR) sequencing revealed a notable rise in BCR diversity among mice immunized with AL. These results indicate that Ag85A-LpqH can be a promising vaccine candidate for tuberculosis prevention and control.

Keywords: biological sciences; immunology; microbiology; natural sciences.