Issue 35, 2024

Feasibility of nitride-based nanocages for the targeted delivery of ifosfamide: a DFT exploration

Abstract

Cancer is one of the most serious health issues and the second leading cause of death after heart disease. Targeted delivery of anticancer drugs via nanocages can help overcome the challenges of cancer treatment. With the help of the quantum mechanical DFT approach, this work describes a theoretical investigation of the absorption mechanism of the anticancer drug ifosfamide (C7H15Cl2N2O2P) in different group III–V nitride-based nanocages, such as B12N12, Al12N12, Ga12N12, and In12N12, to understand the feasibility of nitride-based nanocages for the targeted delivery of the ifosfamide (IFO) drug. Absorption energy analysis reveals that GaNNC exhibits 18.9%, 1.3%, and 0.6% better absorption intensity than BNNC, AlNNC, and InNNC, respectively, toward IFO, which is also supported by the adsorbing distance parameter. The IR spectrum supports the natural formation of the absorbed–absorbent complex as no imaginary frequency was observed. Analysis of different electronic and thermodynamic properties confirms the electronic and thermodynamic suitability of the complexes and supports the previous analyses. Finally, considering all factors such as high structural stability, biocompatibility, greater absorption intensity, along with favorable electronic and thermodynamic stability, Ga12N12 is more suitable than B12N12, Al12N12, and In12N12 nanocages for the targeted delivery of the ifosfamide (C7H15Cl2N2O2P) anticancer drug.

Graphical abstract: Feasibility of nitride-based nanocages for the targeted delivery of ifosfamide: a DFT exploration

Article information

Article type
Paper
Submitted
02 Jul 2024
Accepted
03 Aug 2024
First published
23 Aug 2024

New J. Chem., 2024,48, 15599-15609

Feasibility of nitride-based nanocages for the targeted delivery of ifosfamide: a DFT exploration

A. U. Rahman, D. M. Saaduzzaman, S. M. Hasan and Md. K. U. Sikder, New J. Chem., 2024, 48, 15599 DOI: 10.1039/D4NJ02992E

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