The impact of size for liposomes modified with pH-responsive β-glucan derivatives on the initiation of cellular and humoral immune responses in murine models

The impact of size for liposomes modified with pH-responsive β-glucan derivatives on the initiation of cellular and humoral immune responses in murine models

Size is one of the important factors for antigen carriers because it influences cellular interaction, pharmacokinetics, immune cell activation and the types of immune responses. We developed pH-sensitive polysaccharide derivative-modified liposomes as antigen carriers for induction of antigen-specif...

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Bibliographic Details
Main Authors: Shin Yanagihara, Eiji Yuba, Atsushi Harada
Format: Article
Language:English
Published: Taylor & Francis Group 2024-12-01
Series:Biotechnology & Biotechnological Equipment
Subjects:
Liposome
particle size
polysaccharide
antibody production
antitumour effect
immune response
Online Access:https://www.tandfonline.com/doi/10.1080/13102818.2024.2358992
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Summary:Size is one of the important factors for antigen carriers because it influences cellular interaction, pharmacokinetics, immune cell activation and the types of immune responses. We developed pH-sensitive polysaccharide derivative-modified liposomes as antigen carriers for induction of antigen-specific immune responses. For an earlier study, the size of these liposomes was controlled to within 100–200 nm considering the suitable size for endocytosis. However, since most antigen-presenting cells can engulf larger particles, the proper liposome size and its effect on the induction of cellular versus humoral immune responses remains unclear. Here, we examined the effects of polysaccharide derivative-modified liposome size on immune responses. Liposome size was controlled by using an extrusion method by passing liposomes through a polycarbonate membrane of different pore sizes. Small liposomes encapsulating model antigenic protein suppressed antigen-expressing tumour growth effectively and increased the IgG2a/IgG1 ratio early after liposome administration, suggesting that Th1 response was mainly induced. Large liposomes increased antigen-specific IgG1 and IgG2a production for 56 days compared with small liposomes. These results suggest that small liposomes modified with pH-responsive polysaccharide derivatives could be effective for cancer immunotherapy whereas large liposomes could be suitable for induction of antibody production towards vaccination.
ISSN:1310-2818
1314-3530

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