Researchers from the Shalek Lab at the Ragon Institute of Mass General Brigham, MIT, and Harvard, in collaboration with the Broad Institute, have uncovered key insights into how prior Mycobacterium tuberculosis (Mtb) infection primes the immune system for enhanced protection against reinfection. This study, published in Immunity on August 30, used a non-human primate model to demonstrate that previous Mtb infection leads to a durable, protective immune response that is dependent on CD4+ T cells.
The research examined the lungs after an initial Mtb infection and found that having CD4+ T cells present during a second infection makes the lung environment less inflamed. The study showed that CD4+ T cells help change the behavior of CD8+ T cells, reduce the number of certain immune cells called neutrophils, and lower specific immune signals in other cells, indicating a shift toward a more regulated immune response.
These findings open new avenues for developing vaccines and therapeutics that not only target lymphocytes but also modulate innate immune cells, offering promising strategies to limit tuberculosis disease and improve patient outcomes.