2D/2D Z-scheme WO3/g-C3N4 heterojunctions for photocatalytic organic pollutant degradation and nitrogen fixation
文献信息
Yasi Li, Junkai Wang
Two-dimensional/two-dimensional (2D/2D) Z-scheme WO3/g-C3N4 heterojunctions were successfully prepared by facile rapid calcination, which exhibited considerable photocatalytic performance in environmental application and energy application without any cocatalyst. The synthesized 2D/2D Z-scheme WO3/g-C3N4 significantly improved the visible-light photocatalytic degradation of tetracycline hydrochloride (TC-HCl), and 40%WO3/g-C3N4 had the best photocatalytic degradation effect. 40%WO3/g-C3N4 could also degrade rhodamine B (RhB), methylene blue (MB) and methyl orange (MO), and RhB was almost completely degraded after 20 min irradiation. ˙O2− was the main active species in the degradation process of 40%WO3/g-C3N4. The 2D/2D Z-scheme heterostructure enhanced the photogenerated electron–hole separation and transfer ability and possessed good photocatalytic stability. The 2D/2D Z-scheme WO3/g-C3N4 heterojunction system was first used in nitrogen fixation. 40%WO3/g-C3N4 can simultaneously achieve photocatalytic nitrogen reduction reaction (NRR) and nitrogen oxidation reaction (NOR) to produce NH4+ and NO3−, respectively, using air as a nitrogen source. However, in the presence of a hole sacrificial agent and N2 as a nitrogen source, the photocatalytic nitrogen fixation reaction of 40%WO3/g-C3N4 was dominated by NRR. The nitrogen fixation products and their possible mechanisms were also discussed. This study confirms that the designed 2D/2D Z-scheme WO3/g-C3N4 heterojunctions have great potential in the photocatalytic degradation of different-type organic pollutants and regulable photocatalytic NRR and NOR reactions.
期刊推荐

Proceedings of the National Academy of Sciences of the United States of America

Journal of Physics and Chemistry of Solids

Kinetics and Catalysis

Russian Chemical Reviews

Journal of Catalysis

Organic Preparations and Procedures International

Science Progress

Nature

Molecular Pharmacology

Journal of Medicinal Chemistry
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