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The Bio-oxidation Pattern As a Tool to Study Biodegradation with On-line Measurement

The Bio-oxidation Pattern As a Tool to Study Biodegradation with On-line Measurement. Jongtai Jung (Professor/Ph. D). Major of Environmental Engineering College of Urban Science , University of Incheon. Factors to be considered (in biodegradation study). – Target compound

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The Bio-oxidation Pattern As a Tool to Study Biodegradation with On-line Measurement

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  1. The Bio-oxidation Pattern As a Tool to Study Biodegradation with On-line Measurement • Jongtai Jung • (Professor/Ph. D) • Major of Environmental Engineering • College of Urban Science, University of Incheon

  2. Factors to be considered • (in biodegradation study) • – Target compound • – Microorganism • – Reactor type • – Parameters to be measured • – Analysis method • – The way to enhance reaction • etc.

  3. Determination of biodegradability • Determination of biodegradability of an organic • toxic compound can be a lengthy procedure due to • cumbersome analytical steps for the organic • compound. • The research work which takes long time can be • shortened to answer the most basic question about • response of the bioculture when challenged with • an unknown compound.

  4. Oxygen Uptake and biodegradability • Biochemical oxygen demand(BOD) is a measurement of amount • of dissolved oxygen required to oxidize an organic chemical by • microorganisms • Among the techniques for respirometeric and direct oxygen uptake • measurements, the ones most often used are the manometric and • direct oxygen uptake measurements using galvanic cells oxygen • probes or polarographic electrodes. • The polarographic technique which uses a galvanic cell oxygen probe • is better and simpler technique which when used properly can provide • quick measurement of oxygen uptake rates. • For aerobic process, determination of biodegradability of an organic • toxic compound can be done by on-line monitoring of dissolved • oxygen(DO) and pH level

  5. Purpose of this work • To demonstrate the effectiveness of monitoring • DO, pH and monitoring the bio-oxidation pattern • of an immobilized cell bioreactor. • This bio-oxidation pattern will show that • whether the unknown compound can be biodegraded • or not, and how long it will take for the unknown • compound to be completely biodegraded

  6. Experimental Set-up(1) 1) Recirculation flow-type bioreactor, - Reactor size : 6.4 cm in diameter 20 cm in length.. 2) Reservoir - Reservoir size : 11.4 cm in diameter 25.4 cm in length 3) Total reaction volume - 2 liters including the reservoir.

  7. Experimental Set-up(2) 1) Culture medium - 100 ppm MgCl2, - 0.5 ppm FeCl3 - 10 ppm MgSO4, - 10 ppm K2PO4 • Oxygen supply - Air (1.5 liter/min for EG, TEG) - H2O2 (1% v/v for MMA, Styrene) • Recirculation flow rate : 325ml/min. • Chosen Substrate - MMA(Methyl methacylate), Styrene - Ethylene Glycol(EG), Tetraethylene Glycol(TEG)

  8. Microorganism • Activated sludge(Mixed microbial population) • from Waste water treatment plant • 100 g alginate-immobilized activated sludge • How to immobilize • - Distilled water • - Concentrated sludge(50 mg dry biomass/ g of pallet) • - 0.5% sodium chloride • - 1% sodium alginate • - 0.1 mol/liter CaCl2 • - Distilled water and Conc. Pellets in a ratio 5:2 mixed • with NaCl and Sodium Alginate in a blender • - The homogeneous cell suspension was then extruded • using a syringe pump into CaCl2 solution to obtain the • immobilized bacterial beads

  9. Experiments to be performed(1) 1) Time based control - Oxygen is supplied periodically by a timer - No matter what concentration is, it’s control is the supplying air as an oxygen source for certain period of time and then turning it off for another period of time in consistant bases. - The ups and downs in the DO profile are due to intermittent supply of air which was turned on and off by a timer.

  10. Experiments to be performed(2) 1) Time based control - Since the reactor was operated in batch mode, the oxygen consumption and requirement changed along with substrate concentration. - Consequently the DO level is never constant, but always varied. It decreased slowly, and passed through a minimum before rising back to the original level. - This typical pattern may be observed.

  11. Experiments to be performed(3) 2) Set point control - The DO levels are maintained using a set point control logic with a minimum error bound. - No matter how much time is consumed , set point control is the supplying H2O2 used as an oxygen source till a certain concentration which is already set and automatically turning it off

  12. Experiments to be performed(4) 2) Set point control - The controller has capabilities to perform A/D(analog to digital) conversion, do real time graphing of input variables, and to do data logging. - The microprocessor based controller was obtained from Omega Engineering, This was necessary to determine the consumptions for substrate by keeping the DO level essentially constant.

  13. Analytical Methods • Dissolved Oxygen concentration : • - Clark-type dissolved oxygen probe • -Chart recorder. • 2) MMA, Styrene, EG, TEG Concentration : • - Perkin Elmer8500 Gas Chromatograph, • -Detector : FID • pH : • - pH probe (Orion Cat. No. 91-04) • - pH meter (Corning Model 250, NY)

  14. Fig 1. Experimental set-up of the bioreactor

  15. Results& Discussions on Time Based Control(1) • Fig.2 shows DO profile and methyl methacylate(MMA) • concentration profile in an experiment to study MMA • biodegradation. • The key is an unique pattern(initiation, acceleration, • completion) of the DO curve which forms upon • injection of a substrate

  16. Fig 2. Oxygen Conc. pattern with Time based Control on MMA biodegradation, AB: normal, B: injection, BC : initiation, CD: acceleration, DE: completion

  17. Results& Discussions on Time Based Control(2) • - Section AB shows the baseline DO consumption rates • in absence of any organic compound. • Supply of DO by air was controlled on a time basis. • In this case the DO level dropped initially on injection • of MMA at point B and remained in a consultant range • from 2.5 to 4ppm(CD, acceleration) until concentration • of MMA reached 5ppm before rising up to normal level • from 6.7 to 7.7ppm(DE, completion).

  18. Results& Discussions on Time Based Control(3) • The disappearance of MMA coincides with rising • in DO levels. • In this experiment pH was also monitored and • it showed same trends as that shown by DO profile • including the initiation, acceleration and completion of • the reaction(Fig.3). • The fall in pH value is due to CO2which is a byproduct • of biodegradation reaction while aerating the medium • the pH would rise because CO2 was being displaced.

  19. Fig 3. pH pattern with Time Based Control on MMA biodegradation AB: normal, B: injection, BC: initiation, CD: acceleration, DE: completion

  20. Results& Discussions on Time based Control (4) • At point B in Fig.3, 100ppm MMA was injected • in the reservoir, which initiated a sharp increase • in the product of CO2(BC). • For the next about 7 hours, reaction rate acceleration • as seen by the decrease in MMA concentration • as well as a decrease in the overall pH level. • After 7 hours, the pH level started rising back to the • baseline level, and the MMA concentration was reduced • to less than 1ppm. • Section DE indicates completion of the reaction. • The disappearance of MMA coincides with rise in pH.

  21. Results& Discussions on Set Point Control(1) • Fig.4 shows biodegradation of styrene(50ppm) and the associated • DO and pH profiles. • It should be noted here that since styrene is highly volatile. • Air was not used as a source of DO. Instead hydrogen peroxide • was used • DO level were maintained by a set point control method using • a commercially available data acquisition and control package. • The set point in this case was set to 7.6ppm DO with 0.01ppm • error bound. • But the variation in DO levels from the set point resulted from • error bound and system lag phase until oxygen senor sensed in • chamber the pumped H2O2, mixed in the reservoir.

  22. Fig 4. Oxygen conc. pattern with Set Point Control injected styrene and hydrogen peroxide as substrate and oxygen source, AB: normal, b: injection, BC: initiation, CD: acceleration, DE: completion.

  23. Results& Discussions on Set Point Control (1) • As seen in the Fig.4, the variation in DO levels from the set point • is more when the system is operating without the organic substrate. • This is because when H2O2 is injected (When DO goes below • 7.6ppm) the overall DO concentration attains higher levels • since there is no significant consumption of DO in the absence of • any organic substrate. • When styrene was injected at point B, the slowly DO variation • from the set point decreases because as oxygen was being • generated at the same time it was also consumed due to the • presence of styrene. • The section CD indicates acceleration of the reaction.

  24. Results& Discussions on Set Point Control (2) • Later when the styrene is essentially degraded the variation • in DO level from set point relations to the original values. • Thetime of disappearance of styrene and rise in DO level coincide • and indicates that the reaction is complete without formation of • intermediates.

  25. Results& Discussions on Set Point Control (3) • The change in pH in this case is different from that seen • in MMA experiments. • Here the pH begins to fall and does not rise up to its original • value at the end of the experiment. This happens because any CO2 • that is generated does not leave the system. • At point B, 50ppm styrene was injected in the reservoir, • which initiated a sharp increase in the product of CO2(BC).

  26. Results& Discussions on Set Point Control (4) • For the next about 7 hours, reaction rate accelerated as seen • by the decrease in the overall pH level as well as the decrease • in MMA concentration. • After 7 hours, the pH level does not rise back to the baseline level, • even though the MMA concentration was reduced to less than • 1ppm. • Section DE indicates completion of the reaction. It is shown that • the slope on decreasing pH level is different on each stages. • - There the pH reaches a constant of the reaction.

  27. Pattern with partial oxidation(1) • Fig.5 shows profiles of DO, pH and ethylene glycol • during experiments to study degradation of ethylene glycol. • - As before the DO profile shows trends of initiation, • acceleration, and completion. But this time the rise in DO • doesn't coincide with the disappearance of ethylene glycol. • - Ethylene glycol disappears in 160 min. before DO levels • rise back to normal. • This trend indicates a different degradation mechanism • where intermediates are formed. • In this case ethylene glycol was being converted to formaldehyde • and as a result DO levels remained low until the formaldehyde • was also degraded. • - The formation of formaldehyde was confirmed by GC analysis.

  28. Fig 5. Oxygen conc. and pH pattern with Time Based Control on ethylene glycol biodegradation, AB: normal, B: injection, BC: initiation, CD: acceleration, DC: completion.

  29. GC peak when the only defined medium was injected

  30. GC peak when the only defined medium with ethylene glycol was injected without biomass.

  31. GC peak at 10 minutes after injection of ethylene glycol

  32. GC peak at 25 minutes after injection of ethylene glycol

  33. GC peak at 40 minutes after injection of ethylene glycol

  34. GC peak at 150 minutes after injection of ethylene glycol

  35. GC peak at 300 minutes after injection of ethylene glycol

  36. GC peak after biodegradation is over

  37. Pattern with partial oxidation(2) • Fig.6 provides solution to our original objective which was to • develop an on-line method to follow biodegradation • experiments without analysis of the organic substrate. • In the final experiment with tetraethylene glycol(100ppm) • it was demonstrated how this can be done. • - The profiles of DO and pH follow identical patterns as seen • in earlier case. The regions of reaction initiation acceleration • and completion can be clearly seen. • Tetraethylene glycol was degraded and its rate of degradation • was computed without its analysis. • In this experiment whole reaction time 660 minutes means • the time while TEG itself and all intermediates which can be • biodegraded are degraded.

  38. Fig 6. Oxygen concentration and pH pattern with Time Based Control on TEG biodegradation, AB: normal, B: injection, BC: initiation, CD: acceleration, DC: completion

  39. Conclusions (1) The bio-oxidation pattern on biodegradation of organic compound in real time which has initiation and acceleration completion stages through monitoring DO and pH using on-line measurement with time based and set point control technique. From these profiles the degradation rates of the organic compounds in question can be estimated easily. It is shown that this pattern can be applied on biodegradation with partial oxidation too.

  40. Conclusions (2) 4) It is a tool that not only gives a good estimate of the oxygen demand for a given organic substrate but also it takes in less time than that required in BOD. This tool can be used as an easy and inexpensive technique to control and monitor biological wastewater treatment processes.

  41. Conclusions (3) 5) It can overcome the disadvantages of conventional oxygen uptake measurement with their low resolution in time and provides a method mainly for the use under dynamic process conditions.

  42. Thank you very much for listening

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