Dynamic imaging data are currently analyzed with a tracer-kinetic theory developed for individual time curves measured over whole organs. The assumption is that voxels represent isolated systems which all receive indicator through the same arterial inlet. This leads to well-known systematic errors, but also fails to exploit the spatial structure of the data. In this study, a more general theoretical framework is developed which makes full use of the specific structure of image data. The theory encodes the fact that voxels receive indicator from their immediate neighbors rather than from an upstream arterial input. This results in a tracer-kinetic field theory where the tissue parameters are functions of space which can be measured by analyzing the temporal and spatial patterns in the concentrations. The implications are evaluated through a number of field models for common tissue types. The key benefits of a tracer-kinetic field theory are that: 1) long-standing systematic errors can be corrected, specifically the issue of bolus dispersion and the contamination of large-vessel blood flow on tissue perfusion measurements; 2) additional tissue parameters can be measured that characterize convective or diffusive exchange between voxels; 3) the need to measure a separate arterial input function can be eliminated.

• 出版日期2014-4