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Volume 17, Number 15, Issue of August 1, 1997 pp. 5792-5797
Copyright ©1997 Society for NeuroscienceRequirement for Tyrosine Phosphatase during Serotonergic Neuromodulation by Protein Kinase C
Stefano Catarsi and Pierre Drapeau Centre for Research in Neuroscience, McGill University, and Montreal General Hospital Research Institute, Montreal, Quebec, Canada H3G 1A4
ABSTRACT
Tyrosine kinases and phosphatases are abundant in the nervous system, where they signal cellular differentiation, mediate the responses to growth factors, and direct neurite outgrowth during development. Tyrosine phosphorylation can also alter ion channel activity, but its physiological significance remains unclear. In an identified leech mechanosensory neuron, the ubiquitous neuromodulator serotonin increases the activity of a cation channel by activating protein kinase C (PKC), resulting in membrane depolarization and modulation of the receptive field properties. We observed that the effects on isolated neurons and channels were blocked by inhibiting tyrosine phosphatases. Serotonergic stimulation of PKC thus activates a tyrosine phosphatase activity associated with the channels, which reverses their constitutive inhibition by tyrosine phosphorylation, representing a novel form of neuromodulation.
Key words: single channel; serotonin; protein kinase C; tyrosine phosphorylation; identified neuron; leech
INTRODUCTION
Regulation of ion channel activity by protein phosphorylation is a common mechanism of neuromodulation of transmitter-activated and voltage-gated ion channels (Kaczmarek and Levitan, 1987
). The best characterized actions are those of the serine/threonine kinases activated by calcium or cyclic nucleotides, whose transient effects are terminated by dephosphorylation by protein phosphatases. More recently, tyrosine phosphorylation has been observed for various ligand-gated channels (Hopfield et al., 1988
5-HT is a modulator of neurons in a wide variety of species (Peroutka, 1993
These observations suggest a constitutive suppression of channel activity by tyrosine phosphorylation. We tested for an interaction between PKC and tyrosine dephosphorylation during serotonergic modulation by treating cultured P cells or isolated membrane patches with vanadate, an inhibitor of tyrosine phosphatases (Swarup et al., 1982
MATERIALS AND METHODS
P cells were isolated from Hirudo medicinalis and cultured as described previously (Dietzel et al., 1986. 5-HT was applied by pressure ejection (15 psi) from a pipette with a tip opening of 5 µm. Sodium pervanadate was prepared freshly by mixing 1 part 500 mM H2O2 with 50 parts 10 mM sodium orthovanadate dissolved in saline; the solution was incubated for 15 min at room temperature to reduce H2O2 (Wallace, 1995
Cell-attached recordings of cation channels were obtained as described previously (Drapeau, 1990 3 dB), digitized at 10 kHz, and stored for later analysis using pClamp software (Axon Instruments, Foster City, CA).
Inside-out recordings were obtained as described previously (Catarsi and Drapeau, 1992
RESULTS
As a measure of its macroscopic effect, 5-HT (1 mM) was applied briefly (for 100 msec) onto P cells in culture while the membrane potential was recorded with an intracellular microelectrode. As shown in Figure 1A,B, this resulted in a prolonged depolarization (lasting several seconds) of the P cells (peak depolarization of 3.1 mV ± 0.5; n = 14). When the P cells were exposed to sodium pervanadate (100 µM), a membrane-permeant form of vanadate, before testing the response to 5-HT, this resulted in a significant suppression of the depolarization (0.4 mV ± 0.2; n = 12; p < 0.001 by ANOVA) (Fig. 1A,B). Pervanadate applied alone did not affect the physiological properties of the P cells (Aniksztejn et al., 1997
Fig. 1. Effect of pervanadate on P cell depolarization by 5-HT. A, The net voltage response (relative to the resting potential of
[View Larger Version of this Image (21K GIF file)]
Our previous work has shown that the depolarizing response to 5-HT is attributable to activation of cation channels by PKC, which increases the frequency of channel openings without affecting the mean open time or current amplitude (Drapeau, 1990 
Fig. 2. Effect of pervanadate on PMA activation of cation channels in cell-attached patches. A, Current traces (20 sec) of cation channel activity at the resting potential in a cell-attached patch before (left) and after (right) application of 0.5 µM PMA (indicated by the arrow). Note that PMA increased the number of channel openings. The current amplitude, probability of channel opening (Po), and mean open times (MOTs) were
[View Larger Version of this Image (19K GIF file)]
To examine whether inhibition of tyrosine phosphatases could suppress PKC modulation of cation channels isolated from P cells, we excised membrane patches in the inside-out configuration. When patches were held at a potential of 50 mV (i.e., 
Fig. 3. Effect of orthovanadate on PKC activation of cation channels in inside-out patches. A, Current traces (20 sec) of cation channel activity at 50 mV (i.e.,
[View Larger Version of this Image (20K GIF file)]
Fig. 4. Top. A, Current traces (20 sec) of cation channel activity at 50 mV in an inside-out patch excised from a P cell treated with 0.5 µM PMA before (left) and after (right) application of 50 nM PTPase (indicated by the arrow). Note that no variation of channel activity was observed. The values for current amplitude, Po, and MOT were 3.1 pA, 0.1157 and 1.36 msec before, and 3.2 pA, 0.0880 and 1.83 msec after addition of PTPase. B, Current traces (20 sec) of cation channel activity at 50 mV in an inside-out patch excised from a P cell treated with 0.5 µM PMA before (left) and after (right) application of 100 µM orthovanadate (indicated by the arrow). Note that no variation in channel activity was observed. The values for current amplitude, Po, and MOT were 3.4 pA, 0.0596 and 1.52 msec before, and 3.4 pA, 0.0741 and 1.77 msec after addition of orthovanadate. C. Histogram summarizing the ratio of Po after relative to before (Po/Po control) treatments with PTPase (left) or orthovanadate (middle) in PMA, and PMA in 30 µM genistein (right).
[View Larger Version of this Image (34K GIF file)]
We next examined whether PKC and tyrosine phosphatase activities had additive effects or acted sequentially, i.e., with PKC activating a tyrosine phosphatase. As shown previously (Aniksztejn et al., 1997
DISCUSSION
Our results show that the stimulation of cation channels by 5-HT, or by its intracellular mediator PKC, is blocked when tyrosine phosphatases are inhibited, suggesting that reversal of constitutive tyrosine phosphorylation increases the activity of these channels (Fig. 5). Because this is also true for channels in isolated membrane patches, the simplest interpretation is that a tyrosine phosphatase is closely associated with the channels in the patch and is activated by PKC, as has been shown for some tyrosine phosphatases (Zor et al., 1993
Fig. 5. A model for neuromodulation by tyrosine dephosphorylation. Under resting conditions, cation channels are constitutively tyrosine phosphorylated. 5-HT stimulates PKC, which in turn activates a protein tyrosine phosphatase (PTPase) closely associated with the channels, resulting in their dephosphorylation and increased activity.
[View Larger Version of this Image (17K GIF file)]
Tyrosine phosphorylation is emerging as an important signal not only for early events during cellular differentiation (Cantley et al., 1991
FOOTNOTES
Received March 7, 1997; revised May 6, 1997; accepted May 20, 1997.
This work was supported by a Medical Research Council (MRC) of Canada Fellowship to S.C. and by a Fonds de la Recherche en Santé du Québec Senior Research Scholarship and Medical Research Council grant to P.D. We thank P. V. Nguyen for his critical reading of this manuscript.
Correspondence should be addressed to Dr. Pierre Drapeau, Department of Neurology, Montreal General Hospital, 1650 Cedar Avenue, Montreal, Quebec, Canada H3G 1A4.
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Copyright ©1997 Society for Neuroscience 0270-6474/1997/175792-06$05.00/0
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