Issue 7, 2019

TGase-induced intracellular aggregation of Fe3O4 nanoparticles for increased retention and enhanced T2 MRI

Abstract

Superparamagnetic iron oxides (SPIO) are attractive MRI contrast agents but suffer from limited sensitivity and low tumor specificity. In this study, two sets of SPIO nanoparticles (SPIONPs) were synthesized that were designed to selectively crosslink upon sensing transglutaminase (TGase), which is highly expressed at tumor site, thereby leading to the formation of SPIO nanocluster with T2 signal enhancement properties. For this purpose, SPIONPs with glutamine and lysine surfaces were synthesized. In vitro studies showed that the SPIONPs could crosslink to form aggregates with diameter of 1.3 μm in the presence of TGase and showed a 1.8 fold enhancement in r2 relaxivity compared with the dispersed state. The cellular uptake results illustrated that the SPIONPs could crosslink in high TGase expressing HeLa cells and showed an aggregation-induced retention effect compared with the controlled MCF-7 cell-line (about 1.9 fold). Simultaneously, the administration of the SPIONPs in the HeLa tumor-bearing mice verified the TGase-responsive aggregation and tumor enrichment of the nano contrast agent. MRI imaging also demonstrated the T2 signal enhancing ability of the TGase-responsive SPIONPs; the ΔT2 signal of the SPIONPs in the HeLa tumor-bearing group was about 2.3 fold higher than the MCF-7 group and the TGase-inhibitor treated group.

Graphical abstract: TGase-induced intracellular aggregation of Fe3O4 nanoparticles for increased retention and enhanced T2 MRI

Supplementary files

Article information

Article type
Research Article
Submitted
16 Mar 2019
Accepted
27 Apr 2019
First published
29 Apr 2019

Mater. Chem. Front., 2019,3, 1365-1374

TGase-induced intracellular aggregation of Fe3O4 nanoparticles for increased retention and enhanced T2 MRI

X. Gao, Y. Liu, Y. Li, X. Niu, J. Cao, X. Li, Y. Zhang, D. Tan, W. Wang and Z. Yuan, Mater. Chem. Front., 2019, 3, 1365 DOI: 10.1039/C9QM00159J

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