Facile Transfer Hydrogenation of N-Heteroarenes and Nitroarenes Using Magnetically Recoverable Pd@SPIONs Catalyst.
Huda S AlghamdiAfnan M AjeebiMd Abdul AzizAtif Saeed AlzahraniM Nasiruzzaman ShaikhPublished in: ACS omega (2024)
Catalysts with active, selective, and reusable features are desirable for sustainable development. The present investigation involved the synthesis and characterization of bear-surfaced ultrasmall Pd particles (<1 nm) loaded onto the surface of magnetic nanoparticles (8-10 nm). The amount of Pd loading onto the surface of magnetite is recorded as 2.8 wt %. The characterization process covered the utilization of scanning electron microscopy (SEM), energy-dispersive spectroscopy (EDS), transmission electron microscopy (TEM), inductively coupled plasma (ICP), and X-ray photoelectron spectroscopy (XPS) methods. The Pd@Fe 3 O 4 catalyst has shown remarkable efficacy in the hydrogenation of quinoline, resulting in the production of >99% N-ring hydrogenated (py-THQ) product. Additionally, the catalyst facilitated the conversion of nitroarenes into their corresponding aniline derivatives, where hydrogen was achieved by H 2 O molecules with the aid of tetrahydroxydiboron (THDB) as an equilibrium supportive at 80 °C in 1 h. The high efficiency of a transfer hydrogenation catalyst is closely related to the metal-support synergistic effect. The broader scope of functional group tolerance is evaluated. The potential mechanism underlying the hydrogenation process has been elucidated through the utilization of isotopic labeling investigations. The application of the heterocyclic compound hydrogenation reaction is extended to formulate the medicinally important tubular polymerization inhibitor drug synthesis. The investigation of the recyclability of Pd@Fe 3 O 4 has been conducted.
Keyphrases
- electron microscopy
- highly efficient
- ionic liquid
- reduced graphene oxide
- metal organic framework
- room temperature
- visible light
- high efficiency
- high resolution
- carbon dioxide
- magnetic nanoparticles
- drug delivery
- single molecule
- emergency department
- magnetic resonance imaging
- gold nanoparticles
- computed tomography
- molecular dynamics
- magnetic resonance
- solid state
- mass spectrometry
- simultaneous determination