Link above is only to the abstract:

Abstract Traditional vaccines target specific pathogens, limiting their scope against diverse respiratory threats. We describe an intranasal liposomal formulation combining toll-like receptor (TLR) 4 and 7/8 ligands with a model antigen, ovalbumin, that provided broad, durable protection in mice for at least 3 months against infection with SARS-CoV-2 and Staphylococcus aureus. In addition, the vaccine protected mice from other viruses (SARS-CoV-2, SARS, SCH014 coronavirus), bacteria (Acinetobacter baumannii), and allergens. Protection was mediated by persistent ovalbumin-specific CD4+ and CD8+ memory T cells that imprinted alveolar macrophages (AMs), enhancing antigen presentation and antiviral immunity. Following infection, vaccinated mice mounted rapid pathogen-specific T cell and antibody responses and formed ectopic lymphoid structures in the lung. These results reveal a class of “universal vaccines” against diverse respiratory 🩹

The cool thing about this is the stimulation of CD4 & CD8+ memory cells imprinting alveolar (the alveoli of the lungs) macrophages, a type of Tissue Resident Macrophage (TRMs) that will then hang out in that location, where the invaders first appeared, waiting for them to return. Whereupon they will alert the immune system that “those guys” are back, you know what to do. I heard the process explained this way:

TRMs are like that cowboy seemingly snoozing away, at the Old Saloon. Then when “those infectious guys” that had infected one before, and markers for them are imprinted on the TRMs show up, suddenly the guy snoozing away ‘wakes up’, saying “I remember YOU!” and alerts The Posse (Immune System) that it’s time to take action. The version I heard on TWIV was a bit cuter, but I edited this for clarity.