Liver cancer has been identified as the second most common cause of cancer-related mortality. Routine liver diagnosis by recording magnetic resonance (MR) images in the presence of a liver-directing contrast agent (CA) can recognize any abnormalities early. However, the clinically approved liver-specific Gd(III)-based CAs are of great concern for bio-safety. In fact, several medical agencies have restricted the usage of such CAs. Thus, to develop non-Gd-based biocompatible CAs for liver imaging, a thermodynamically stable and kinetically inert nonaquated six-coordinate paramagnetic Fe(III)-complex (1) is confined within a biocompatible porous silica nanoparticle of size about 18 nm. Such entrapment has boosted the longitudinal relaxivity value of Complex 1 (r1 = 0.59 × 10-3 m-1s-1) upto 9 times to 5.36 × 10-3 m-1s-1, which further increased to 10.83 × 10-3 m-1s-1 in the presence of 0.67 × 10-3 m concentration of serum albumin protein. Surface functionalization of the nanoparticle with hydrophobic p-methoxybenzamide (C1@SiO2-PMBA-NP) facilitates HepG2 cell internalization as evinced by in vitro fluorescent images and flow cytometry analyses. Time-dependent contrast changes in the liver MR images recorded on C57BL/6 mice in a preclinical MRI instrument establish the applicability of the biocompatible C1@SiO2-PMBA-NP as the T1-weighted liver-directing CA for magnetic resonance imaging (MRI).
Liver-Directing Fe(III)-Based MRI Contrast Agent.
Geetanjali Deka,Arisha Arora,Priyanka Bhat,Vandna Singh,Hari Mohan,S. Kumaran,C. Mukherjee
Published 2025 in Small
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- Publication year
2025
- Venue
Small
- Publication date
2025-08-13
- Fields of study
Medicine, Chemistry
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Semantic Scholar, PubMed
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