4.7 Article

Competition for electrons between pyridine and quinoline during their simultaneous biodegradation

期刊

ENVIRONMENTAL SCIENCE AND POLLUTION RESEARCH
卷 24, 期 32, 页码 25082-25091

出版社

SPRINGER HEIDELBERG
DOI: 10.1007/s11356-017-0082-3

关键词

Pyridine; Quinoline; Mono-oxygenation reaction; Electron donors; Affinity

资金

  1. ability construction project of local Colleges and Universities in Shanghai [16070503000]
  2. Special Fund of State Key Joint Laboratory of Environment Simulation and Pollution Control [16K10ESPCT]
  3. Shanghai Gaofeng and Gaoyuan Project for University Academic Program Development
  4. US National Science Foundation [0651794]
  5. Div Of Chem, Bioeng, Env, & Transp Sys
  6. Directorate For Engineering [0651794] Funding Source: National Science Foundation

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Biodegradation of pyridine and quinoline is initiated with mono-oxygenation reactions that require an intracellular electron donor. Simultaneous biodegradation of both substrates should set up competition for the intracellular electron donor that may inhibit one or more of the mono-oxygenation steps. An internal circulation baffled biofilm reactor (ICBBR) was used to evaluate the impacts of competition during pyridine and quinoline biodegradation. Compared with independent biodegradation, pyridine and quinoline removal rates were slowed when biodegraded simultaneously, although the pyridine removal rate decreased more than for quinoline. The first mono-oxygenation of quinoline (to 2-hydroxyquinoline) always was faster than the first mono-oxygenation of pyridine (to 2-hydroxypyridine), and the difference was accentuated with pyridine and quinoline which were biodegraded simultaneously due to the competition for intracellular electron donor. Competition also existed between the second mono-oxygenations, and the removal rate of 2-hydroxypyridine was faster than the rate for 2-hydroxyquinoline, even though the rate was faster for quinoline than pyridine. Adding an exogenous electron donor accelerated all mono-oxygenations in proportion to the amount of donor added, but the increments were greater for quinoline due to its higher affinity for intracellular electron donors than pyridine. When actual coking wastewater was used as the background matrix, removals of pyridine and quinoline exhibited the same competitive trends.

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