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Vol. 281, Issue 3, 1211-1218, 1997
Sherrington School of Physiology, UMDS, St. Thomas Hospital Campus,
London SE1 7EH, UK
The transport of azidodeoxythymidine (AZT) into and within the central
nervous system (CNS) has special clinical significance due to the
ability of AZT to alleviate certain neurological symptoms associated
with the acquired immunodeficiency syndrome (AIDS). AZT was thought to
be similar to its parent compound, thymidine, in that it entered the
CNS via the choroid plexuses (blood-CSF barrier) and
could not cross the blood-brain barrier (BBB). However, a saturable
transport system for thymidine at the BBB has recently been identified.
The aim of this study was to test the hypothesis that AZT follows its
physiological counterpart in its mode of entry into and movement within
the CNS. Initial experiments using the in situ brain
perfusion technique indicated that the blood-to-CNS transfer constants
for [3H]AZT (blood-to-cerebrum; 0.95 ± 0.12 µl/min/g) were significantly lower than those determined for
[3H]thymidine. Also, [3H]AZT entered the
CNS purely by a diffusive process. The movement of
[3H]AZT within the CNS was further investigated by a
ventriculocisternal perfusion technique and indicated that the majority
of intraventricularly perfused [3H]AZT remained within
the ventricles (79.9%), with little escaping to blood (14.1 ± 3.1%) or brain (6.0 ± 1.3%). Overall, these results suggest
that the choroid plexus/CSF pathway was unlikely to be solely
responsible for the levels of [3H]AZT observed in brain
and that the BBB plays a significant role in the brain entry of this
analog. However, in contrast to thymidine, AZT enters the CNS purely by
a diffusional process.
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