AI Article Synopsis

  • Researchers developed uniform-sized clodronate-encapsulated liposome nanoplatforms to enhance macrophage depletion for immunotherapy, addressing limitations of previous formulations.
  • The new liposomes were functionalized for targeted delivery and labeled for in vivo imaging, demonstrating stability and effective biodistribution in tests.
  • Among the four types created, the mannosylated liposome showed superior ability to deplete M2 macrophages in both normal liver and tumor settings, indicating its potential as an effective treatment option.

Article Abstract

Background: Immunotherapy with clodronate-encapsulated liposomes, which induce macrophage depletion, has been studied extensively. However, previously reported liposomal formulation-based drugs (Clodrosome and m-Clodrosome) are limited by their inconsistent size and therapeutic efficacy. Thus, we aimed to achieve consistent therapeutic effects by effectively depleting macrophages with uniform-sized liposomes.

Results: We developed four types of click chemistry-based liposome nanoplatforms that were uniformly sized and encapsulated with clodronate, for effective macrophage depletion, followed by conjugation with Man-N and radiolabeling. Functionalization with Man-N improves the specific targeting of M2 macrophages, and radioisotope labeling enables in vivo imaging of the liposome nanoplatforms. The functionalized liposome nanoplatforms are stable under physiological conditions. The difference in the biodistribution of the four liposome nanoplatforms in vivo were recorded using positron emission tomography imaging. Among the four platforms, the clodronate-encapsulated mannosylated liposome effectively depleted M2 macrophages in the normal liver and tumor microenvironment ex vivo compared to that by Clodrosome and m-Clodrosome.

Conclusion: The newly-developed liposome nanoplatform, with finely tuned size control, high in vivo stability, and excellent ex vivo M2 macrophage targeting and depletion effects, is a promising macrophage-depleting agent.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10903058PMC
http://dx.doi.org/10.1186/s12951-024-02325-7DOI Listing

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