Issue 11, 2024

Albumin nanocapsules and nanocrystals for efficient intracellular drug release

Abstract

In order to achieve a therapeutic effect, many drugs have to reach specific cellular compartments. Nanoscale drug delivery systems extend the circulation time, reduce adverse effects and thus improve tolerability compared to systemic administration. We have developed two types of albumin-coated nanocarriers equipped with built-in dyes to track their cellular uptake and intracellular enzymatic opening. Using the approved antiprotozoal drug and STAT3 inhibitor Atovaquone (Ato) as prototype for a hydrophobic small molecule, we show that Ato-loaded ovalbumin-coated nanocapsules (Ato-nCap) preferentially enter human myeloid cells. In contrast, Ato nanocrystals coated with human serum albumin (Ato-nCry) distribute their cargo in all different immune cell types, including T and B cells. By measuring the effect of Ato nanocarriers on induced STAT3 phosphorylation in IL-10-primed human dendritic cells and constitutive STAT3 phosphorylation in human melanoma cells, we demonstrate that the intracellular Ato release is particularly effective from Ato nanocrystals and less toxic than equal doses of free drug. These new nanocarriers thus represent effective systems for intracellular drug delivery.

Graphical abstract: Albumin nanocapsules and nanocrystals for efficient intracellular drug release

Supplementary files

Article information

Article type
Communication
Submitted
12 Apr 2024
Accepted
05 Aug 2024
First published
29 Aug 2024
This article is Open Access
Creative Commons BY license

Nanoscale Horiz., 2024,9, 1978-1989

Albumin nanocapsules and nanocrystals for efficient intracellular drug release

S. P. Chali, J. Westmeier, F. Krebs, S. Jiang, F. P. Neesen, D. Uncuer, M. Schelhaas, S. Grabbe, C. Becker, K. Landfester and K. Steinbrink, Nanoscale Horiz., 2024, 9, 1978 DOI: 10.1039/D4NH00161C

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