AI Article Synopsis

  • Researchers are exploring prolonged antigen delivery systems designed to mimic long-term pathogen exposure to enhance durable immunity.
  • The study utilizes His-tagged proteins that form nanoparticles and microparticles, which disintegrate slowly after being administered subcutaneously, simulating an endocrine-like secretory system for gradual antigen release.
  • Testing on mice and pigs revealed strong immune responses, suggesting these materials could be a new tool for improving immune stimulation and vaccine effectiveness without the need for additional adjuvants.

Article Abstract

Developing prolonged antigen delivery systems that mimic long-term exposure to pathogens appears as a promising but still poorly explored approach to reach durable immunities. In this study, we have used a simple technology by which His-tagged proteins can be assembled, assisted by divalent cations, as supramolecular complexes with progressive complexity, namely protein-only nanoparticles and microparticles. Microparticles produced out of nanoparticles are biomimetics of secretory granules from the mammalian hormonal system. Upon subcutaneous administration, they slowly disintegrate, acting as an endocrine-like secretory system and rendering the building block nanoparticles progressively bioavailable. The performance of such materials, previously validated for drug delivery in oncology, has been tested here regarding the potential for time-prolonged antigen release. This has been completed by taking, as a building block, a nanostructured version of p30, a main structural immunogen from the African swine fever virus (ASFV). By challenging the system in both mice and pigs, we have observed unusually potent pro-inflammatory activity in porcine macrophages, and long-lasting humoral and cellular responses in vivo, which might overcome the need for an adjuvant. The robustness of both innate and adaptive responses tag, for the first time, these dynamic depot materials as a novel and valuable instrument with transversal applicability in immune stimulation and vaccinology.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10934719PMC
http://dx.doi.org/10.3390/nano14050435DOI Listing

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