Whole-body microvascular permeability of small molecules in man: clinical aspects, basic concepts and limitations of the single injection technique
- 1 January 1985
- journal article
- research article
- Published by Taylor & Francis in Scandinavian Journal of Clinical and Laboratory Investigation
- Vol. 45 (6) , 509-513
- https://doi.org/10.3109/00365518509155251
Abstract
In order to estimate whole-body permeability-surface area (PS) product, the initial slope of the plasma disappearance curve was determined after simultaneous i.v. injection of 24Na+ (mol.wt 24) and 51 Cr-EDTA (mol.wt 342). Twelve subjects were studied. Plasma volume (PV) was measured by the indicator dilution method, and the mean transit time of tracer in plasma was calculated as the reciprocal value of the initial fractional disappearance (initial slope). Estimated whole-body PS product (=PV/) of 24Na+ (median 2.72, range 1.51–3.80 ml/min × 100 g body weight) was significantly higher than that of 51Cr-EDTA (median 2.16, range 1.59–2.84 ml/min × 100 g, pna :PS51Cr-EDTA ratio was median 1.26 (range 0.91–1.44), and this value is significantly lower than the ratio between the free aqueous diffusion coefficients (D24Na:D51Cr-EDTA=2.54, pCr-eDTA and earlier estimates of whole-body PS product of polyfructosan (mol.wt 3000) was close to the ratio of their free diffusion coefficients. The results indicate that whole-body PS product may be estimated from the initial slope of the plasma disappearance curve of a tracer, but mixing problems and flow-limited transport, as indicated by a PS ratio below that of the free diffusion coefficients, may be difficult to overcome, especially when using tracers of a low molecular weight.Keywords
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