Abstract Klebsiella pneumoniae (Kp) is a leading cause of hospital- and community-acquired infections and is increasingly resistant to last-line antibiotics, positioning it as a World Health Organization-designated priority pathogen. Vaccine development has been hindered by the extensive diversity of Kp exopolysaccharide capsules. We developed a cellular nanoparticle (CNP) platform in which bacterial outer membrane vesicles (OMVs) are stably coated onto a STING (stimulator of interferon genes)-a
A STING-adjuvanted outer membrane vesicle nanoparticle vaccine vs. Klebsiella pneumoniae elicits broad capsule type cross-protection
Hervé Besançon·Elisabet Bjånes·Kalisa Kang·Samuel Kim·Samira Dahesh·Sydney R. Morrill·Shawn M. Hannah·Anh T. P. Ngo·Liangfang Zhang·Victor Nizet·Daniel Sun