4.6 Article

Continuous measurements of plasma protein extravasation with microdialysis after various inflammatory challenges in rat and mouse skin

Journal

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajpheart.00542.2003

Keywords

inflammation; permeability; microcirculation

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This study describes the use of microdialysis technique for continuous measurement of plasma protein extravasation ( PPE) in rat and mouse skin with drug application either intravenously or via the microdialysis fiber. Hollow plasmapheresis fibers ( 3- cm length, 0.4- mm diameter, cutoff 3,000 kDa) were placed subcutaneously on the back of anesthetized mice and rats. Intravenous injection of dextran ( Macrodex, 60 mg/ ml) increased PPE by 355% from baseline within 30 min in rats with ligated kidneys ( n = 6; P < 0.05) but not in animals with intact kidneys. Phalloidin ( 500 μ g/ kg iv 40 min before dextran, n = 6; P < 0.05) did not change the response to dextran in either group. Animals receiving PGE(1), compound 48/ 80 ( mice), paclitaxel, docetaxel, and cremophor EL via the microdialysis fiber were also provided with a control fiber receiving vehicle. Both rats and mice had constant PPE in the control fiber, and there was no change in PPE in the NaCl- treated groups ( rats, n = 4; mice, n = 6). Application via the fiber of PGE(1) ( 20 mu g/ ml), compound 48/ 80 ( mice; 4 mg/ ml), and docetaxel ( 0.5 mg/ ml) increased PPE compared with baseline within 60 min by 139% ( n = 6; P < 0.05), 273% ( n = 6; P < 0.05), and 325% ( n = 5; P < 0.05), respectively. Phalloidin alone did not increase PPE ( n = 5; P < 0.05). Pretreatment with phalloidin did not inhibit the increase after PGE(1) or compound 48/ 80 but inhibited that after docetaxel ( n = 6). Paclitaxel ( 0.6 mg/ ml, n = 5) or vehicle ( Cremophor) ( n = 5) gave no increase in PPE. The results demonstrate that microdialysis can be used to continuously measure changes in PPE after inflammatory challenges in skin of rats and mice.

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