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Macromolecular structure determination using pulsed electron spin resonance techniques.
Reference
BB/F004583/1
Principal Investigator / Supervisor
Dr William John Ingledew
Co-Investigators /
Co-Supervisors
Professor James Naismith
,
Professor Olav Schiemann
,
Professor Graham Smith
,
Prof. Malcolm White
Institution
University of St Andrews
Department
Biology
Funding type
Research
Value (£)
651,347
Status
Completed
Type
Research Grant
Start date
01/01/2008
End date
30/06/2011
Duration
42 months
Abstract
This proposal seeks to develop and demonstrate advanced new tools for biomolecular characterisation utilising recent major technological advances made in mm-wave technology for pulse electron spin resonance (ESR), developed under the top-rated £2.6M Basic Technology (BT) Program in 2003, 'Bringing the NMR paradigm to ESR'. These advances will allow the combination of GHz excitation bandwidths, nanosecond deadtime, fast phase cycling and high magnetic fields for pulse ESR measurements, which represent remarkable advances on current state-of-the-art, and open up major new opportunities in structural biology. We aim to demonstrate large increases in sensitivity for both DEER and hyperfine techniques, demonstrate new capabilities for efficient polarization transfer in DNP methodologies and show that ESR Fourier Transform techniques can become a standard tool for analysing rapid dynamics and electron transfer reactions in biological systems. A particular focus will be on the development and optimisation of DEER methods to study complex structural interactions (incorporating assembly of complex signalling systems, assembly of DNA binding proteins on DNA, and movement in large intermembraneous complexes). Nitroxide spin labels are placed on cysteines engineered into the proteins (site-directed spin-labelling, SDSL) and the magnetic interactions between adjacent SDSLs (or between an SDSL and an intrinsic paramagnet) allows the measurement of distance. We describe a number of experiments in detail where we have preliminary data and where the whole program is underpinned with modern commercial instrumentation. (Bruker E580 pulsed ESR EleXsys system, X-band and Q-band, ENDOR and ELDOR).
Summary
In biology it is often possible to have a good understanding of the function of a particular biomolecule such as a protein. Biologists have also developed tools that often allow them to understand the sequence of elements that make that protein and understand its overall structure / often in exquisite detail. However, what biology is considerably less good at is relating that proteins structure to its function. It lacks precise tools to understand how proteins or other biomolecules interact with one another and what microscopic changes occur during that interaction. Yet a detailed understanding of this structure/function relationship is vital as it often underpins drug development strategies. One promising emerging methodology to solve that problem uses chemistry to accurately locate tiny magnetic molecules in exactly the same position within each larger biomolecule. Advanced magnetic resonance techniques are then used to derive quantitative information about the local structure and dynamics around those probes as well as using them to understand interactions between proteins, RNA or DNA. In this proposal we wish to demonstrate that using new technologies, recently developed under a major top-rated UK Basic Technology program, we can improve sensitivity and time resolution of these type of measurements by orders of magnitude relative to commercial instrumentation typically costing between £0.5M to more than £1M. We believe that this proposal is outstanding value as all the high risk technologies have already been developed and integrated into a working system. We also have a fully developed and ambitious applications program targeting important problems in biology, where we have preliminary data and where it is completely underpinned by the availability of commercial instrumentation. We thus believe this is a relatively low risk but high reward project that promises provide new and effective tools for biologists seeking to understand structure/function problems.
Committee
Closed Committee - Biomolecular Sciences (BMS)
Research Topics
Structural Biology, Technology and Methods Development
Research Priority
X – Research Priority information not available
Research Initiative
Technology Development Initiative 2 (TDRI2) [2007]
Funding Scheme
X – not Funded via a specific Funding Scheme
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