Leukotriene C4 Transport and Metabolism in the Central Nervous System
- 1 April 1986
- journal article
- research article
- Published by Wiley in Journal of Neurochemistry
- Vol. 46 (4) , 1308-1312
- https://doi.org/10.1111/j.1471-4159.1986.tb00655.x
Abstract
The transport and metabolism of radiolabeled leukotriene (LT) C4 in the CNS were investigated after intraventricular injection. Under thiopental (Pentothal) anesthesia, New Zealand white rabbits were injected intracerebroventricularly with 0.2 ml of artificial CSF containing 2.5 .mu.Ci of [3H]LTC4 (36 Ci/mmol), 0.3 .mu.Ci of [14C] mannitol, and, in some cases, 0.9 mg of probenecid, 1.8 mg of cysteine, 1.4 .mu.g of unlabeled LTC4, or 2 mg of tolazoline HCl. After 2 h, the conscious rabbits were killed, and the quantity and nature of the 3H and 14C were determined in CSF, choroid plexus, and brain. The [3H]LTC4 recovered in CSF and brain was not extensively metabolized, as > 70% of the 3H remained [3H] LTC4, although some spontaneous conversion to 11-trans-[3H]LTC4 occurred. Oxidized forms of [3H] LTC4, [3H]LTD4, and [3H]LTE4 did not exceed 18% in CSF and brain. After intraventricular injection of [3H]LTC4, 3H was transfered from the CSF to blood by a probenecidsensitive, but tolazoline-insensitive, transport system in the CNS much more rapidly than mannitol. Cysteine decreased the retention of [3H]LTC4 in brain. These results are consistent with previous in vitro observations that [3H]LTC4 is transferred from CSF into blood by an efficient transport system for LTC4 in choroid plexus.Keywords
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