In vitro and Bioimaging Studies of Mesoporous Silica Nanocomposites Encapsulated Iron-oxide and Loaded Doxorubicin Drug (DOX/IO@Silica) as Magnetically Guided Drug Delivery System

Hemant Kumar; Balaram Pani; Jitender Kumar; Pramod Kumar

doi:10.2174/1389201023666220428084920

In vitro and Bioimaging Studies of Mesoporous Silica Nanocomposites Encapsulated Iron-oxide and Loaded Doxorubicin Drug (DOX/IO@Silica) as Magnetically Guided Drug Delivery System

Curr Pharm Biotechnol. 2023;24(10):1297-1306. doi: 10.2174/1389201023666220428084920.

Authors

Hemant Kumar^{1

2

3}, Balaram Pani³, Jitender Kumar¹, Pramod Kumar⁴

Affiliations

¹ Department of Chemistry, University of Delhi, Delhi-110007, India.
² Department of Chemistry, Ramjas College, University of Delhi, Delhi, 110007, India.
³ Department of Chemistry, Bhaskaracharya College of Applied Sciences, University of Delhi, Delhi, 110075, India.
⁴ Department of Chemistry and Chemical Sciences, School of Physical and Material Sciences, Eternal University Baru Sahib, Central University of Himachal Pradesh, Dharamshala, Himachal Pradesh, India.

PMID: 37254276
DOI: 10.2174/1389201023666220428084920

Abstract

Background: In recent years, the delivery of drugs by nanocomposites has emerged as an exciting field of research for bio-imaging tools and targeted cancer treatment. The large surface area and porous volume of mesoporous silica nanocomposites (MSN's) have gained a lot of interest for their application in the delivery of drugs and the magnetic properties of iron oxide (IO) nanocomposites play a key role in the targeted delivery system.

Methods: In this study, mesoporous silica encapsulated IO nanocomposites loaded with doxorubicin (DOX) were synthesized for the magnetically guided delivery of anticancer drugs. The synthesis of IO nanocomposites was done through the precipitation method, and then silica encapsulation and drug loading were done by the StÖber method.

Results: The magnetically driven delivery of the drug is produced by the encapsulation of magnetically active IO in the mesoporous silica shell. The controlled release of DOX is possible because of the MSN's. TEM images show that the nanocomposites have a spherical morphology and average diameter in the range of 120 nm. Power-XRD data confirm the crystalline nature of nanocomposites. The strong absorption peak was observed in UV-Visible spectroscopy at 490 nm and quenching in fluorescence spectra confirms the encapsulation of DOX in the mesoporous silica shell. VSM data showed the magnetic nature of nanocomposites, with large magnetic susceptibility (74.88 emu/g). The use of DOX/IO@Silica nanocomposites as a sustainable drug release and targeted drug delivery vehicle has been reported here. The pH dependent release of DOX was studied and significant release was observed at lower pH. In-vitro cell viability assay and fluorescence imaging assay have demonstrated that these nanocomposites show significant dose-dependent toxicity to cancer cells in the presence of a magnetic field.

Conclusion: In-vitro studies via the MTT assay showed that these synthesized nanocomposites in culture are non-toxic to healthy cells compared to DOX-induced cytotoxicity due its controlled release and can be further strengthened by magnetic guidance. Therefore, due to its optical properties and potential for guided delivery of drug to the targeted site, these nanocomposites are ideal as an anticancer agent and bio-imaging prob.

Keywords: (DOX); in-vivo; Mesoporous silica nanocomposites (MSN’s); core-shell iron oxide/silica nanocomposites (IO@Silica); magnetically guided drug delivery; the iron oxide (IO).

MeSH terms

Antineoplastic Agents* / therapeutic use
Delayed-Action Preparations
Doxorubicin / pharmacology
Drug Delivery Systems
Drug Liberation
Iron
Nanocomposites* / chemistry
Nanoparticles* / chemistry
Porosity
Silicon Dioxide / chemistry

Substances

ferric oxide
Delayed-Action Preparations
Silicon Dioxide
Doxorubicin
Antineoplastic Agents
Iron