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The effect of charge and albumin on cellular uptake of supramolecular polymer nanostructures
- Source :
- Journal of Materials Chemistry B vol.12 (2024) date: 2024-05-22 nr.20 p.4854-4866 [ISSN 2050-750X]
- Publication Year :
- 2024
-
Abstract
- Intracellular delivery of functional biomolecules by using supramolecular polymer nanostructures has gained significant interest. Here, various charged supramolecular ureido-pyrimidinone (UPy)-aggregates were designed and formulated via a simple “mix-and-match” method. The cellular internalization of these UPy-aggregates in the presence or absence of serum proteins by phagocytic and non-phagocytic cells, i.e., THP-1 derived macrophages and immortalized human kidney cells (HK-2 cells), was systematically investigated. In the presence of serum proteins the UPy-aggregates were taken up by both types of cells irrespective of the charge properties of the UPy-aggregates, and the UPy-aggregates co-localized with mitochondria of the cells. In the absence of serum proteins only cationic UPy-aggregates could be effectively internalized by THP-1 derived macrophages, and the internalized UPy-aggregates either co-localized with mitochondria or displayed as vesicular structures. While the cationic UPy-aggregates were hardly internalized by HK-2 cells and could only bind to the membrane of HK-2 cells. With adding and increasing the amount of serum albumin in the cell culture medium, the cationic UPy-aggregates were gradually taken up by HK-2 cells without anchoring on the cell membranes. It is proposed that the serum albumin regulates the cellular internalization of UPy-aggregates. These results provide fundamental insights for the fabrication of supramolecular polymer nanostructures for intracellular delivery of therapeutics.
Details
- Database :
- OAIster
- Journal :
- Journal of Materials Chemistry B vol.12 (2024) date: 2024-05-22 nr.20 p.4854-4866 [ISSN 2050-750X]
- Notes :
- Song, Jiankang
- Publication Type :
- Electronic Resource
- Accession number :
- edsoai.on1446904553
- Document Type :
- Electronic Resource