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Title
Revealing the Synergistic Anticancer Efficacy of Curcumin and Iota-Carrageenan-Stabilized Silver Nanoparticles Derived From Solieria robusta
Type Article
Keywords
AgNPs; carrageenan; curcumin; cytotoxicity; drug deliver
Abstract
n this study, a red seaweed (Solieria robusta) containing ι-carrageenan (Carr) was used for nanoparticles (NPs) synthesis using silver (Ag) ions. Initially, the ι-Carr was extracted from S. robusta using the alkali method. Te Carr extracted was fractionated into 3 fractions and > 14 kDa fraction showing high yield with maximum sulfate content characterized using Fourier transform infrared (FT-IR) as ι-Carr was used for AgNPs synthesis. Te synthesized CarrAgNPs were again used for curcumin (Cur) encapsulation. Te cytotoxicity of Carr, Cur, CarrAgNPs, and CurCarrAgNPs was evaluated using HeLa cell lines by MTT assay. Te CarrAgNPs and CurCarrAgNPs were characterized using UV-visible spectroscopy, as well as FT-IR and XRD analysis. Te UV-visible spectrum confrms the CarrAgNPs showing characteristic SPR bands recorded between 344 and 490 nm with broad peak at 430 nm. Te shape of the NPs is spherical, arranged in order of seven per chain. Te XRD and FT-IR characteristics confrm the orthorhombic crystal structure of these NPs. Remarkably, Cur-loaded CarrAgNPs demonstrate potent anticancer properties by maximum reduction of HeLa cell viability after 24 h at 200 μg/mL in pH 7.4 in an MTT assay medium. A signifcant increase in the cancer cell viability was recorded at high concentrations of CurCarrAgNPs, confrming its less difusion and dissolution properties and bioavailability due to lipophilic Cur encapsulation, whereas cytotoxicity was increased proportionately by increasing concentrations of Cur, Carr, and CarrAgNPs that confrm a direct relation with size, dissolution, and bioavailability recorded on the basis of cell death in 24 h of introduction at pH 7.4. Te cytotoxicity results suggest the potential of Cur, Carr, CarrAgNPs, and CurCarrAgNPs for drug delivery in selective biomedical product developments. Tis study highlights the versatility and efectiveness of CurCarrAgNPs in cancer therapy by enhancing the efcacy of therapeutic interventions and targeted drug delivery
Researchers جانسون موهان (First researcher) , Adila Farisa K. M. (Second researcher) , Mohammad Sibtain Kadri (Third researcher) , M. P. Sudhakar (Fourth researcher) , Kulanthaiyesu Arunkumar (Fifth researcher) , gholamreza Abdi (Not in first six researchers)