4.7 Article

ABCC1: a gateway for pharmacological compounds to the ischaemic brain

Journal

BRAIN
Volume 131, Issue -, Pages 2679-2689

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/brain/awn222

Keywords

ABC transporter; blood-brain barrier; neuroprotection; pharmacotherapy; stroke

Funding

  1. Swiss National Center of Competence in Research
  2. Swiss National Science Foundation [3200B0112056/1]
  3. Baasch-Medicus Foundation
  4. Hermann-Klaus Foundation
  5. David-and-Betty-Koetser Foundation

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By preventing access of drugs to the CNS, the blood-brain barrier hampers developments in brain pharmacotherapy. Strong efforts are currently being made to identify drugs that accumulate more efficaciously in ischaemic brain tissue. We identified an ATP-binding cassette (ABC) transporter, ABCC1, which is expressed on the abluminal surface of the brain capillary endothelium and mildly downregulated in response to focal cerebral ischaemia, induced by intraluminal middle cerebral artery occlusion. In biodistribution studies we show that ABCC1 promotes the accumulation of known neuroprotective and neurotoxic compounds in the ischaemic and non-ischaemic brain, ABCC1 deactivation reducing tissue concentrations by up to two orders of magnitude. As such, ABCC1s expression and functionality in the brain differs from the liver, spleen and testis, where ABCC1 is strongly expressed on parenchymal cells, resulting-in case of liver and testis-in directed transport from the tissue into the blood. After focal cerebral ischaemia, ABCC1 deactivation abolished the efficacy of both neuroprotective and neurotoxic compounds. Our data indicate that ABCC1 acts as gateway for pharmacological compounds to the stroke brain. We suggest that the tailoring of compounds binding to abluminal but not luminal ABC transporters may facilitate stroke pharmacotherapy.

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