Evaluating the antimicrobial activity and cytotoxicity of polydopamine capped silver and silver/polydopamine core-shell nanocomposites

Fabrication of bioactive nanomaterials with improved stability and low toxicity towards healthy mammalian cells have recently been a topic of interest. Bioactive metal nanomaterials such as silver nanoparticles (AgNPs) tend to lose their stability with time and become toxic to some extent, limiting their biological applications. AgNPs were separately encapsulated and loaded on the surface of a biocompatible polydopamine (PDA) to produce Ag-PDA and Ag@PDA nanocomposites to unravel the issue of agglomeration. PDA was coated through the self-polymerization of dopamine on the surface of AgNPs to produce Ag-PDA core-shells nanocomposites. For Ag@PDA, PDA spheres were first designed through self-polymerization of dopamine followed by in situ reduction of silver nitrate (AgNO3) without any reductant. AgNPs sizes were controlled by varying the concentration of AgNO3. The TEM micrograms showed monodispersed PDA spheres with an average diameter of 238 nm for Ag-PDA and Ag@PDA nanocomposites. Compared to Ag@PDA, Ag-PDA nanocomposites have shown insignificant toxicity towards human embryonic kidney (HEK-293T) and human dermal fibroblasts (HDF) cells with cell viability of over 95% at concentration of 250 µg/mL. A excellent antimicrobial activity of the nanocomposites was observed; with Ag@PDA possessing bactericidal effect at concentration as low as 12.5 µg/mL. Ag-PDA on the other hand were only found to be bacteriostatic against gram-positive and gram-negative bacteria was also observed.The University of Witwatersrand School of Chemistry, The University of the Witwatersrand Postgraduate Merit Award and the National Research Foundation of South Africa.https://www.journals.elsevier.com/arabian-journal-of-chemistryhj2023Physic

Unraveling the effects of surface functionalization on the catalytic activity of ReSe2 nanostructures towards the hydrogen evolution reaction

Herein, the surface functionalization of ReSe2 nanostructures by surfactants was investigated. This was done to understand how the use of various surfactants affects the catalytic activity of ReSe2 nanostructures towards the hydrogen evolution reaction (HER), and to determine which surfactant would result in maximal exposure of the active edge sites without impeding the catalytic processes of the HER. Oleylamine (OLA), oleic acid (OA), and trioctylphosphine oxide (TOPO) were used as the surfactants. Powder X-ray diffraction confirmed the formation of ReSe2 nanostructures that crystallized in a distorted 1 T phase triclinic system with a P-1 space group. The FTIR, XPS, NMR, and computational studies revealed that the surfactants bind to the surface of the ReSe2 nanostructures through their respective head groups. The ReSe2 nanostructures synthesized using TOPO (ReSe2-TOPO) had the lowest on-set potential, Tafel slope, and overpotential at 10 mA/cm2 at 73 mV, 58 mV/dec, and 171 mV, respectively. The catalytic performance of the nanostructures was significantly affected by their interaction with the surfactants. A high degree of passivation by the surfactant resulted in poor catalytic activity, and a lower degree of passivation resulted in excellent catalytic activity towards the HER