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Vol. 290, Issue 3, 1493-1501, September 1999
Experimental Therapeutics Branch, National Institute of
Neurological Disorders and Stroke, National Institutes of Health,
Bethesda, Maryland
The firing rates of many basal ganglia neurons recorded in awake rats
oscillate at seconds-to-minutes time scales, and the D1/D2 agonist
apomorphine has been shown to robustly modulate these oscillations. The
use of selective D1 and D2 antagonists suggested that both these
receptor subfamilies are involved in apomorphine's effects. In the
present study, spectral analysis revealed that baseline multisecond
oscillations were significantly periodic in 71% of globus pallidus
neurons. Baseline oscillations had a wide range of periods within the
analyzed range, with a population mean of 32 ± 2 s.
Administration of the D1 agonist SKF 81297 (6-chloroPB) at 1.0 or 5.0 mg/kg significantly changed these oscillations, reducing means of
spectral peak periods to 14 to 16 s (i.e., increasing oscillatory
frequency). This effect was attenuated by D2 antagonist pretreatment.
The D2 agonist quinpirole did not cause a significant population change
in multisecond periodicities. The strongest effects on multisecond
periodicities occurred after combined treatment with SKF 81297 and
quinpirole. Low, ineffective doses of SKF 81297 and quinpirole, when
combined, produced a significant increase in oscillatory frequency.
Also, when quinpirole was administered after an already effective dose
of SKF 81297, quinpirole shifted oscillations to an even faster range
(typically to periods of <10 s). The dopaminergic control of
multisecond periodicities in globus pallidus firing rate demonstrates
D1/D2 receptor synergism, in that the effects of D1 agonists are
potentiated by and partially dependent on D2 receptor activity.
Modulation of multisecond oscillations in firing rate represents a
novel means by which dopamine can influence globus pallidus physiology.
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