In this study, various concentrations of strontium (Sr) into a fixed amount of starch (St) and FeO nanostructures (NSs) were synthesized with the co-precipitation approach to evaluate the antibacterial and photocatalytic properties of the concerned NSs. The study aimed to synthesize nanorods of FeO with co-precipitation to enhance the bactericidal behavior with dopant-dependent FeO. Advanced techniques were utilized to investigate the structural characteristics, morphological properties, optical absorption and emission, and elemental composition properties of synthesized samples. Measurements via X-ray diffraction confirmed the rhombohedral structure for FeO. Fourier-transform infrared analysis explored the vibrational and rotational modes of the O-H functional group and the C=C and Fe-O functional groups. The energy band gap of the synthesized samples was observed in the range of 2.78-3.15 eV, which indicates that the blue shift in the absorption spectra of FeO and Sr/St-FeO was identified with UV-vis spectroscopy. The emission spectra were obtained through photoluminescence spectroscopy, and the elements in the materials were determined using energy-dispersive X-ray spectroscopy analysis. High-resolution transmission electron microscopy micrographs showed NSs that exhibit nanorods (NRs), and upon doping, agglomeration of NRs and nanoparticles was observed. Efficient degradations of methylene blue increased the photocatalytic activity in the implantation of Sr/St on FeO NRs. The antibacterial potential for and was measured against ciprofloxacin. bacteria exhibit inhibition zones of 3.55 and 4.60 mm at low and high doses, respectively. shows the measurement of inhibition zones for low and high doses of prepared samples at 0.47 and 2.40 mm, respectively. The prepared nanocatalyst showed remarkable antibacterial action against bacteria rather than at high and low doses compared to ciprofloxacin. The best-docked conformation of the dihydrofolate reductase enzyme against for Sr/St-FeO showed H-bonding interactions with Ile-94, Tyr-100, Tyr-111, Trp-30, ASP-27, Thr-113, and Ala-6.
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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9979251 | PMC |
http://dx.doi.org/10.1021/acsomega.2c07980 | DOI Listing |
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