Development of Folate‐Superparamagnetic Nanoconjugates for Inhibition of Cancer Cell Proliferation

Author:

Ferjaoui Zied1,Nahle Sara1,Schneider Raphaël2,Kerdjoudj Halima3,Mertz Damien4,Quilès Fabienne5,Ferji Khalid6ORCID,Gaffet Eric1,Alem Halima17ORCID

Affiliation:

1. Université de Lorraine CNRS IJL (UMR 7198) F‐54000 Nancy France

2. Université de Lorraine CNRS LRGP (UMR 7274) F‐54000 Nancy France

3. Université de Reims Champagne Ardenne Biomatériaux et Inflammation en Site Osseux (BIOS) EA 4691 F‐51100 Reims France

4. Université de Strasbourg CNRS Institut de Physique et Chimie des Matériaux de Strasbourg (UMR 7504) F‐67034 Strasbourg France

5. Université de Lorraine CNRS LCPME (UMR 7564) F‐54000 Nancy France

6. Université de Lorraine CNRS LCPM (UMR 7375) F‐54000 Nancy France

7. Institut Universitaire de France Nancy France

Abstract

AbstractHere, a versatile strategy to engineer smart theranostic nanocarriers is reported. The core/shell nanosystem is composed of a superparamagnetic iron oxide (Fe3−δO4) nanoparticle (NP) core bearing the biocompatible thermo‐responsive poly(2‐(2‐methoxy)ethyl methacrylate‐oligo(ethylene glycol methacrylate), P(MEO2MAx‐OEGMA100−x) copolymer (where x and 100‐x represent the molar fractions of MEO2MA and OEGMA, respectively). Folic acid (FA) is end‐conjugated to the P(MEO2MAx‐OEGMA100−x) copolymer, leading to Fe3δO4@P(MEO2MAx‐OEGMA100−x)‐FA, to facilitate active targeting of NPs to cancer cells. A highly potent hydrophobic anticancer agent doxorubicin (DOX) is incorporated in the thermo‐responsive P(MEO2MAx‐OEGMAy) brushes via supramolecular interactions to increase its solubility and the assessment of therapeutic potentials. These experiments confirm the magnetic hyperthermia properties of nanocarrier and reveal that only a small amount (10% ± 4%) of DOX is diffused at room temperature, while almost full drug (100%) is released after 52 h at 41 °C. Interestingly, it is found that P(MEO2MA60‐OEGMA40) polymers offer to NPs a promising stealth behavior against Human Serum Albumin and Fibrinogen model proteins.

Publisher

Wiley

Subject

Mechanical Engineering,Mechanics of Materials

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