Issue 3, 2025

PEGylation of indium phosphide quantum dots prevents quantum dot mediated platelet activation

Abstract

Quantum dots (QDs) are semiconducting inorganic nanocrystals, that have garnered interest in biological and medical spheres due, to their potential benefits in biomedical imaging and drug-delivery systems. Indium phosphide QDs shelled with zinc sulphide (InP/ZnS) are viewed as more biocompatible than previous heavy metal based QDs. However, little is known about how InP/ZnS QDs affect a key blood cell, the platelet. Understanding how platelets interact with QDs is critical as unwanted activation can lead to pathological thrombus formation. Herein, we demonstrate PEGylation of InP/ZnS QDs coated with lipoic acid (QD-LA) or coated with penicillamine (QD-Pen) surface ligands induced markedly less platelet aggregation, platelet–QD interactions, integrin activation, alpha granule secretion and restored platelet spreading in washed platelets in comparison to their non-PEGylated counterparts. Furthermore, in whole blood, PEGylation of QDs reduced the number of QDs in the thrombus, thereby helping to minimise the chance of dysfunctional thrombus formation. Overall, we show that QD PEGylation is important to help prevent QD mediated platelet activation. In combination with the most biocompatible coating, PEGylation markedly reduced platelet activation, widening the concentrations at which QDs were viable for development as potential drug delivery or imaging agents.

Graphical abstract: PEGylation of indium phosphide quantum dots prevents quantum dot mediated platelet activation

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Article information

Article type
Paper
Submitted
18 Jun 2024
Accepted
07 Nov 2024
First published
05 Dec 2024
This article is Open Access
Creative Commons BY license

J. Mater. Chem. B, 2025,13, 1052-1063

PEGylation of indium phosphide quantum dots prevents quantum dot mediated platelet activation

L. Naylor-Adamson, T. W. Price, Z. Booth, S. V. L. Leonard, J. Gallo, L. D. Tung, S. Harvell-Smith, N. Thi Kim Thanh, Z. Aslam, D. Allsup, N. Hondow, T. Chamberlain, J. E. Schneider, K. Naseem, J. G. Bouillard, G. J. Stasiuk and S. D. J. Calaminus, J. Mater. Chem. B, 2025, 13, 1052 DOI: 10.1039/D4TB01334D

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