J Neurophysiol (December 1, 2002). 10.1152/jn.00078.2002
Submitted on 5 February 2002
Accepted on 12 August 2002
Local Application of Dopamine Inhibits Pyramidal Tract Neuron
Activity in the Rodent Motor Cortex
Patrick W.
Awenowicz1 and
Linda L.
Porter1,2
1Program in Neuroscience and
2Department of Anatomy, Physiology, and
Genetics, Uniformed Services University of the Health Sciences,
Bethesda, Maryland 20814
Awenowicz, Patrick W. and
Linda L. Porter.
Local Application of Dopamine Inhibits Pyramidal Tract Neuron
Activity in the Rodent Motor Cortex. J. Neurophysiol. 88: 3439-3451, 2002. Cortical neurons respond in
a variety of ways to locally applied dopamine, perhaps because of the
activation of different receptors within or among subpopulations of
cells. This study was conducted to assess the effects of dopamine and
the receptor subtypes that mediate the responses of a specific
population of neurons, the pyramidal tract neurons (PTNs) in the rodent
motor cortex. The specific subfamilies of dopamine receptors expressed by PTNs also were determined. PTNs were identified by antidromic stimulation in intact animals. Extracellular recordings of their spontaneous activity and glutamate-induced excitation were performed with multi-barrel pipettes to allow simultaneous recording and iontophoresis of several drugs. Prolonged (30 s) application of dopamine caused a progressive, nonlinear decrease in spontaneous firing
rates for nearly all PTNs, with significant reductions from baseline
spontaneous activity (71% of baseline levels) occurring between 20 and
30 s of iontophoresis. The D1 selective (SCH23390) and the D2
selective (eticlopride) antagonists were both effective in blocking
dopamine-induced inhibition in nearly all PTNs. Mean firing levels were
maintained within 3% of baseline levels during co-application of the
D1 antagonist with dopamine and within 11% of baseline levels during
co-application of the D2 antagonist and dopamine. SCH23390 was
ineffective however, in 2 of 16 PTNs, and eticlopride was ineffective
in 3 PTNs. The dopamine blockade by both antagonists in most neurons,
along with the selective blockade by one, but not the other antagonist
in a few neurons indicate that the overall population of PTNs exhibits
a heterogeneous expression of dopamine receptors. The firing rate of
PTNs was significantly enhanced by iontophoresis of glutamate
(mean = 141% of baseline levels). These increases were
attenuated significantly (mean= 98% of baseline) by
co-application with dopamine in all PTNs, indicating dopaminergic
interactions with glutamate transmission. The expression of dopamine
receptors was studied with dual-labeling techniques. PTNs were
identified by retrograde labeling with fast blue and the D1a, D2, or D5
receptor proteins were stained immunohistochemically. Some, but not all
PTNs, showed labeling for D1a, D2, or D5 receptors. The D1a and D2
receptor immunoreactivity was observed primarily in the somata of PTNs,
whereas D5 immunoreactivity extended well into the apical dendrites of
PTNs. In accordance with findings of D1 and D2 receptor antagonism of
dopamine's actions, the identification of three DA receptor subtypes
on PTNs suggests that dopamine can directly modulate PTN activity
through one or more receptor subtypes.
