This research develops targeted lipid nanoparticle delivery systems to improve tuberculosis treatment and vaccination. By replacing PEG coatings and using mannose to target infected macrophages, it aims to deliver drugs more effectively, reduce treatment duration, improve vaccine performance, and contribute to the global elimination of tuberculosis.
Tuberculosis remains deadly despite relying on decades-old antibiotics. This research uses computational methods to identify immune response similarities between TB and other diseases, enabling drug repurposing. By borrowing already approved treatments, this approach aims to restore immune balance, combat drug resistance, and accelerate the development of new TB therapies.