4.7 Article

Dendrimer-conjugated iron oxide nanoparticles as stimuli-responsive drug carriers for thermally-activated chemotherapy of cancer

Journal

COLLOIDS AND SURFACES B-BIOINTERFACES
Volume 155, Issue -, Pages 182-192

Publisher

ELSEVIER SCIENCE BV
DOI: 10.1016/j.colsurfb.2017.04.025

Keywords

Cancer; Combination therapy; Dendrimers; Doxorubicin; Drug delivery; Iron oxide nanoparticles; Magnetic hyperthermia; PAMAM

Funding

  1. IITB-Monash Research Academy
  2. Nanomission of DST, Govt. of India

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In recent years, functional nanomaterials have found an appreciable place in the understanding and treatment of cancer. This work demonstrates the fabrication and characterization of a new class of cationic, biocompatible, peptide dendrimers, which were then used for stabilizing and functionalizing magnetite nanoparticles for combinatorial therapy of cancer. The synthesized peptide dendrimers have an edge over the widely used PAMAM dendrimers due to better biocompatibility and negligible cytotoxicity of their degradation products. The surface engineering efficacy of the peptide dendrimers and their potential use as drug carriers were compared with their PAMAM counterparts. The peptide dendrimer was found to be as efficient as PAMAM dendrimers in its drug-carrying capacity, while its drug release profiles substantially exceeded those of PAMAM's. A dose-dependent study was carried out to assess their half maximal inhibitory concentration (IC50) in vitro with various cancer cell lines. A cervical cancer cell line that was incubated with these dendritic nanoparticles was exposed to alternating current magnetic field (ACMF) to investigate the effect of elevated temperatures on the live cell population. The DOX-loaded formulations, in combination with the ACMF, were also assessed for their synergistic effects on the cancer cells for combinatorial therapy. The results established the peptide dendrimer as an efficient alternative to PAMAM, which can be used successfully in biomedical applications. (C) 2017 Elsevier B.V. All rights reserved.

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