EPSRC Reference: |
EP/H020446/1 |
Title: |
Adsorption of catechols at TiO2 single crystal surfaces.Charge transfer processes in photovoltaics and structure of novel biomedical materials. |
Principal Investigator: |
THOMAS, Dr AG |
Other Investigators: |
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Researcher Co-Investigators: |
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Project Partners: |
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Department: |
Physics and Astronomy |
Organisation: |
University of Manchester, The |
Scheme: |
Overseas Travel Grants (OTGS) |
Starts: |
18 September 2009 |
Ends: |
17 December 2009 |
Value (£): |
4,259
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EPSRC Research Topic Classifications: |
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EPSRC Industrial Sector Classifications: |
No relevance to Underpinning Sectors |
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Related Grants: |
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Panel History: |
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Summary on Grant Application Form |
This project will study the interaction of two molecules from a group of ring molecules called catechols, namely pyrocatechol and dopamine, with titanium dioxide (TiO2) surfaces. This interaction is of some interest for two reasons. Firstly it has been known for about 10 years or so that pyrocatechol (and other catechols including dopamine) adsorbed on TiO2 nanoparticles shifts the absorption of light from the ultraviolet region to the visible region of the electromagnetic spectrum. Since TiO2 is so cheap this may offer the potential for new cheap solar generation of electricity. It has been suggested in these types of cells, where a molecule is attached to a semiconductor surface that the strength of attachment is key in the efficient transfer of charge from the molecule to the surface. The other problem is that TiO2 is a photocatalyst capable of decomposing certain organic molecules so clearly the long term stability of the molecule must be understood and verified before this type of technology is developed. In addition, the catechol-TiO2 system is of interest as a possible targeted biomedical material. Unlike catechol, dopamine has a small chain on the side of the ring which can be grafted onto other molecules. In this way the dopamine can be attached to the surface of TiO2 nanoparticles and these functional molecules attached to the chain. Careful selection of the functional molecules can allow the nanoparticle TiO2 to respond to a specific stimulus. A polymer chain - Polytheyleneglycol (PEG) - effectively renders the nanoparticles invisible to the body's immune system. The inclusion of grafted temperature sensitive molecules along with the PEG means that at the site of an infection or disease the nanoparticles will clump together and form an opaque region in an x-ray. Since the particles are small they can be injected - thus quickly giving a surgeon information on where a problem may be located. Again one of the potential problems in these particles is the stability. We have been working with colleagues in the School of Pharmacy at Manchester, looking at the real nanoparticle systems but the surface structure is complicated by the presence of solvents and molecules used in the synthesis of the particles and chains. In this work we will use atomically clean surfaces and deposit carefully controlled amounts of pure catechols. Using the radiation facility at Elettra on Trieste we can determine a number of things about the nature of the chemistry at the surface including the orientation of the molecules and their stability over short timescales and different conditions. X-ray photoemission and absorption spectroscopies will be used to determine changes to the chemistry over time. In addition using a combination of x-ray absorption and photoemission we are able to infer the charge transfer time between the adsorbed molecules and the surface of the TiO2. We will study adsorption two different surfaces of TiO2 i.e. the rutile (110) and anatase (101), which arise from different crystal structures of TiO2. Anatase is the structure adopted by nanoparticulate TiO2 so our studies on this crystal will potentially give more realistic information. Rutile is a more widely studied material as it is easier to grow and obtain commercially. In fact we are one of the few groups who have carried out substantial research on anatase single crystal surfaces. Although some of what we have determined in previous work suggests organic acid molecules interact in similar ways on these two surfaces it is of some fundamental interest to determine whether this is also the case for the catechols. In addition the two different molecules will allow us to determine whether the presence of the side chain on the dopamine results in differences in the adsorption geometry or the chemical stability since this chain could potential react with the oxygen molecule through which the dopamine bonds to the surface.
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Key Findings |
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Potential use in non-academic contexts |
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Description |
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Summary |
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Date Materialised |
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Sectors submitted by the Researcher |
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Project URL: |
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Further Information: |
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Organisation Website: |
http://www.man.ac.uk |