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Location of Solubilization of 2′-ethylhexyl Salicylate in Micelles
Institution:1. Department of Automation, Xiamen University, Xiamen 361005, Fujian, China;2. School of Information Technology, York University, Toronto M3J 1P3, Canada;3. College of Physics and Electronic Engineering Information, Wenzhou University, Wenzhou 325035, Zhejiang, China;4. Innovation Center for Cell Biology, Xiamen University, Xiamen 361102, Fujian, China;1. Instituto de Ciencias Marinas de Andalucía (CSIC), Campus Universitario Río San Pedro, 11519 Puerto Real, Cádiz, Spain;2. CEI-MAR International Campus of Excellence of the Sea, Spain;3. Departamento de Química-Física, Facultad de Ciencias del Mar y Ambientales, Universidad de Cádiz, Campus Río San Pedro s/n, Puerto Real, Cádiz 11510, Spain;4. Ecología Funcional de Sistemas Acuáticos, Centro Universitario Regional Este, Universidad de la República, Rocha, Uruguay;5. Instituto Español de Oceanografía, Centro Oceanográfico de Cádiz, Puerto Pesquero, Muelle de Levante s/n, 11006 Cádiz, Spain;6. IFAPA Centro El Toruño, Camino Tiro de Pichón s/n, 11500 El Puerto de Santa María, Spain
Abstract:Absorption and excited state intramolecular proton transfer (ESIPT) fluorescence of 2′-ethylhexyl salicylate (EHS) were examined in the presence of cationic, non-ionic, and anionic surfactants. It was found that linear EHS molecule was solubilized in micelles with its flexible and hydrophobic 2′-ethylhexyl chain toward the micellar core and with its rigid salicyl moiety toward the micelle-water interface. The UV absorption of EHS was improved and the intramolecular hydrogen bonding formation of EHS was favored, resulting in greatly enhanced ESIPT fluorescence. The excited EHS molecules decay via visible luminescence and non-radiative deactivation. The binding sites of EHS in micelles were explained at a molecular level in terms of molecular structures and sizes of EHS and surfactants. Dynamic fluorescence quenching and spectral measurements of ester hydrolysis of EHS provide further evidences for the binding sites of EHS in different micelles.
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