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Developmental differences in the expression of ABC transporters at rat brain barrier interfaces following chronic exposure to diallyl sulfide. | LitMetric

AI Article Synopsis

  • Many pregnant women and prematurely born infants need medications for conditions like cancer and psychiatric disorders, raising concerns about drug transfer across the blood-brain barrier (BBB) during development.
  • Eight types of ATP-binding cassette (ABC) transporters were studied in postnatal rats to understand their expression and activity in the liver, brain, and choroid plexus, especially after chronic treatment with a known inducer, diallyl sulfide (DAS).
  • Results showed that ABC transporter expression varies by tissue type and age, highlighting the BBB's ability to adaptively regulate its defense mechanisms against foreign substances throughout development.

Article Abstract

Many pregnant women and prematurely born infants require medication for clinical conditions including cancer, cardiac defects and psychiatric disorders. In adults drug transfer from blood into brain is mostly restricted by efflux mechanisms (ATP-binding cassette, ABC transporters). These mechanisms have been little studied during brain development. Here expression of eight ABC transporters (abcb1a, abcb1b, abcg2, abcc1, abcc2, abcc3, abcc4, abcc5) and activity of conjugating enzyme glutathione-s-transferase (GST) were measured in livers, brain cortices (blood-brain-barrier) and choroid plexuses (blood-cerebrospinal fluid, CSF, barrier) during postnatal rat development. Controls were compared to animals chronically injected (4 days, 200 mg/kg/day) with known abcb1a inducer diallyl sulfide (DAS). Results reveal both tissue- and age-dependent regulation. In liver abcb1a and abcc3 were up-regulated at all ages. In cortex abcb1a/b, abcg2 and abcc4/abcc5 were up-regulated in adults only, while in choroid plexus abcb1a and abcc2 were up-regulated only at P14. DAS treatment increased GST activity in livers, but not in cortex or choroid plexuses. Immunocytochemistry of ABC transporters at the CSF-brain interface showed that PGP and BCRP predominated in neuroepithelium while MRP2/4/5 were prominent in adult ependyma. These results indicate an age-related capacity of brain barriers to dynamically regulate their defence mechanisms when chronically challenged by xenobiotic compounds.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6461637PMC
http://dx.doi.org/10.1038/s41598-019-42402-8DOI Listing

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