Selective blood-tumor barrier disruption by leukotrienes

Abstract

✓ The authors have previously reported that intracarotid infusion of 5 µg leukotriene C₄ (LTC₄) selectively increases blood-tumor barrier permeability in rat RG-2 tumors. In this study, rats harboring RG-2 tumors were given 15-minute intracarotid infusions of LTC₄ at concentrations ranging from 0.5 µg to 50.0 µg (seven rats in each dose group). Blood-tumor and blood-brain barrier permeability were determined by quantitative autoradiography using ¹⁴C aminoisobutyric acid. The transfer constant for permeability (K_i) within the tumors was increased twofold by LTC₄ doses of 2.5, 5.0, and 50.0 µg compared to vehicle alone (90.00 ±21.14, 92.68 ± 15.04, and 80.17 ± 16.15 vs. 39.37 ± 6.45 µl/gm/min, respectively; mean ± standard deviation; p < 0.01). No significant change in K_i within the tumors was observed at the 0.5-µg LTC₄ dose. Blood-brain barrier permeability was selectively increased within the tumors. At no dose in this study did leukotrienes increase permeability within normal brain. To determine the duration of increased opening of the blood-tumor barrier by LTC₄ administration, K_i was measured at 15, 30, and 60 minutes after termination of a 15-minute LTC₄ infusion (seven rats at each time point). The mean K_i value was still high at 15 minutes (92.68 ± 15.04 µl/gm/min), but declined at 30 minutes (56.58 ± 12.50 µl/gm/min) and 60 minutes (55.40 ± 8.10 µl/gm/min) after the end of LTC₄ infusion. Sulfidopeptide leukotrienes LTC₄, LTD₄, LTE₄ and LTF₄ were infused to compare their potency in opening the blood-tumor barrier. The mean leukotriene E₄ was the most potent, increasing the permeability value 37½ fold compared with vehicle alone (139.86 ± 23.95 vs. 39.37 ± 6.45 µl/gm/min).