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4 - PGSE measurements in complex and exchanging systems

Published online by Cambridge University Press:  06 August 2010

William S. Price
Affiliation:
University of Western Sydney
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Summary

Introduction

A requirement in measuring transport (e.g., transmembrane) or exchange (e.g., ligand binding) is to be able to identify a measurable NMR parameter that has a different value in each state. Modulation of this parameter by the transport or exchange process is examined to characterise the process. Traditionally, NMR chemical shifts or relaxation times have been used for this purpose. With the advent of PGSE methods, a difference in diffusion properties (i.e., a difference in diffusion coefficient between sites or a difference in motional restriction) becomes another measurable NMR parameter that can be used to probe transport or exchange.

In the simplest case the exchange will occur between two freely diffusing sites (e.g., a ligand binding to a macromolecule; Figure 4.1); however, in many real systems (e.g., a suspension of biological cells) one site, or both sites if at higher cellular volume fractions, may be restricted. In contrast to the previous chapter where only simple restricting systems with reflecting boundary conditions were considered and the diffusing species did not interact with other restricting geometries, in real systems (e.g., biological cells, porous systems) it may also be necessary to consider the effects of a combination of exchange, restriction, obstruction and polydispersity in addition to surface and bulk relaxation as well as different bulk diffusion coefficients in each medium (e.g., Figure 4.2). As a consequence, modelling such systems can be very complicated and various approximations are necessarily used.

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NMR Studies of Translational Motion
Principles and Applications
, pp. 147 - 184
Publisher: Cambridge University Press
Print publication year: 2009

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