PRESSURE REVERSED EXTRACELLULAR STRIATAL DOPAMINE DECREASE PRODUCED BY D(1)-RECEPTOR AGONIST SKF-38393, AND D(2)-RECEPTOR AGONIST LY-171555, BUT FAILED TO CHANGE THE EFFECT OF THE ACTIVATION OF BOTH D(1)-RECEPTOR AND D(2)-RECEPTOR

被引：28

作者：

ABRAINI, JH

FECHTALI, T

ROSTAIN, JC

机构：

[1] Laboratoire de biologie des hautes pressions, CNRS URA 1330, Faculté de médecine nord, 13326 Marseille cédex 15, boulevard Pierre Dramard

来源：

NEUROSCIENCE | 1992年 / 50卷 / 02期

关键词：

D O I：

10.1016/0306-4522(92)90432-2

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

When human divers or experimental animals are exposed to high pressure, they develop the high-pressure neurological syndrome which is characterized by electroencephalographic changes, and behavioral disturbances. Recently, neurochemical disorders such as a pressure-induced increase in dopamine release have been demonstrated. In the present study, pharmacological experiments, using dopamine receptor agonists such as D1 receptor agonist SKF 38393, D2 receptor agonist LY 171555, and D1/D2 receptor agonist apomorphine, were performed to investigate dopamine receptor function at the neurochemical level. Only apomorphine and mixed SKF 38393 + LY 171555 prevented the pressure-induced increase in dopamine release while SKF 38393 or LY 171555 administered alone failed to do so. The results suggest that the D1-D2 link would be reduced under high pressure because of an abnormal function of D1 receptors which would allow high-affinity D2 states for dopamine. If so, such a preponderance of high-affinity states in D2 postsynaptic receptors could be associated with hyperbaric hyperlocomotor activity. Elsewhere, results also suggested that the pressure-induced disorders in dopamine receptor function could be involved in the pressure-induced elevation in dopamine release.

引用

页码：395 / 402

页数：8

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