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The Journal of Neuroscience, February 15, 2003, 23(4):1099
BRIEF COMMUNICATION
Dynamic Modulation of Inspiratory Drive Currents by Protein Kinase A and Protein Phosphatases in Functionally Active MotoneuronsChristopher M. Bocchiaro1, Shane A. Saywell2, and Jack L. Feldman2 Systems Neurobiology Laboratory, Departments of 1 Physiological Science and 2 Neurobiology, David Geffen School of Medicine, University of California Los Angeles, Los Angeles, California 90095-1763
ABSTRACT
TOP
ABSTRACT
Introduction
Plasticity underlying adaptive, long-term changes in breathing behavior is hypothesized to be attributable to the modulation of respiratory motoneurons by intracellular second-messenger cascades. In quiescent preparations, protein kinases, including cAMP-dependent protein kinase A (PKA), potentiate glutamatergic inputs. However, the dynamic role of protein kinases or phosphatases in functionally active and behaviorally relevant preparations largely remains to be established. Rhythmic inspiratory drive to motoneurons innervating inspiratory muscles is mediated by the release of glutamate acting predominately on AMPA receptors. In rhythmically active brainstem slices from neonatal rats, we investigated whether synaptic AMPA receptor function could be modulated by changes in intracellular PKA activity, affecting inspiratory drive in hypoglossal (XII) motoneurons. Intracellular perfusion of the catalytic subunit of PKA potentiated endogenous synaptic and (exogenously applied) AMPA-induced currents in XII motoneurons. Conversely, when a peptide inhibitor of PKA was perfused intracellularly, inspiratory drive currents were depressed. Intracellular perfusion with microcystin, a potent phosphatase 1 and 2a inhibitor, increased both endogenous and exogenous AMPA receptor-mediated currents, further supporting a role of phosphorylation in modulating motoneuronal excitability affecting behaviorally relevant synaptic inputs. These findings suggest that PKA is constitutively active in XII motoneurons in vitro. Thus, endogenous synaptic AMPA currents in XII motoneurons are influenced by phosphorylation, specifically by PKA, and dephosphorylation. The role of this modulation may be to keep the activity of motoneurons within a dynamic range that aids in responding to different physiological challenges affecting breathing, such as exercise, hypoxia, and sleep.
Key words: excitability; respiration; preBötzinger; plasticity; PKA; AMPA; phosphatase; sleep apnea
Introduction
Established models of neuronal plasticity, such as long-term potentiation (LTP) and long-term depression (LTD) seen in hippocampal, cerebellar, and cortical neurons (Colwell and Levine, 1995
; Kameyama et al., 1998
In quiescent preparations, protein kinases, including PKA, potentiate glutamatergic inputs; however, the dynamic role of protein kinases or phosphatases in functionally active and behaviorally relevant neurons largely remains to be established. Motoneurons receive excitatory amino acid input from premotor neurons and transform this activity into appropriate output to produce muscle contraction. Delineating how motoneuronal excitability is controlled is an important component in understanding behavior (Rekling et al., 2000
The principal fast excitatory inputs to motoneurons, like most other neurons, are glutamatergic (Rekling et al., 2000
XII motoneurons receive inspiratory-related excitatory drive currents that are principally mediated by AMPA receptors (Funk et al., 1993
Materials and Methods
Experiments were performed on a medullary slice preparation that spontaneously generates respiratory rhythm (Smith et al., 1991
Electrophysiological recording. XII motoneurons were visualized with infrared differential interference contrast microscopy. XII motoneurons were identified by the criteria of Funk et al. (1993)
; ~1.5 µm tip diameter) were pulled from borosilicate glass on a horizontal puller. Electrodes were filled with solution containing (in mM): 120 potassium gluconate, 11 EGTA, 5 NaCl, 1 CaCl2, 10 HEPES, and 2 ATP (Mg2+ salt), pH adjusted to 7.3 with KOH. Positive pressure was applied to the back of the electrode as it was advanced into the tissue. When the electrode was positioned on the surface of the soma of the target neuron, positive pressure was released and negative pressure was applied to form a Giga
70 mV.
Respiratory-related nerve activity was recorded from the cut ends of the XII nerve (XIIn) with a suction electrode, amplified 10,000 or 20,000 times, bandpass filtered (3-3000 Hz), and rectified. XIIn burst activity defined the inspiratory period.
Drugs and drug application. The following drugs (obtained from Sigma, St. Louis, MO) were prepared in patch electrode solution: active catalytic subunit of PKA (250 U/ml; P2645; Sigma); inhibitory peptide (PKI) (500 µg/ml; P0300; Sigma), which binds to the catalytic subunit of PKA and inhibits its activity (Raymond et al., 1993
For experiments involving application of exogenous AMPA, action potential-dependent synaptic transmission was prevented by bath application of tetrodotoxin (TTX, 1 µM). AMPA was dissolved in ACSF (10 µM) and pressure ejected from glass electrodes (tip diameter, 3 µm; pressure, 10 psi; duration, 50-150 msec) placed under visual guidance above the neuron being recorded. With this concentration and injection protocol (see below), we did not see any evidence of desensitization of AMPA responses between injections.
Data acquisition and analysis. Signals were recorded digitally (DC, 20 kHz) and stored on a computer hard drive for off-line analysis using Clampfit 8.0 (Axon Instruments) and Origin 6.0 (Origin Lab Corp.). Statistical values are reported as means ± SD. Differences between means were calculated by independent t test, and p < 0.05 was considered significant.
Recordings of endogenous synaptic drive currents were triggered off the onset of the integrated XII motor output. Peak inspiratory drive currents were averaged from 6 to 10 consecutive inspiratory bursts. Averaged peak currents were normalized to current amplitude immediately after whole-cell break-in. After establishing whole-cell patch configuration, membrane currents remained stable for the duration of the experiments, with no significant rundown or change in input resistance.
Results
Effects on endogenous inspiratory drive
When whole-cell voltage-clamped with microelectrodes filled with standard patch solution, XII motoneurons exhibit periodic inward currents in-phase with integrated XII motor output (Funk et al., 1993
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Figure 1. Effects of PKA and phosphatase manipulation on inspiratory drive currents. A, Effect of intracellular dialysis of activated PKA enhanced peak endogenous glutamatergic inspiratory drive currents in XII motoneurons. Potentiation of synaptic drive currents of a PKA dialyzed XII motoneuron 1, 5, and 30 min after establishing whole-cell recording (break-in; Vh =
To establish a role for PKA in modulating endogenous respiratory drive, we included a purified peptide of the PKA catalytic subunit in the patch electrode. This resulted in progressive increases in peak inspiratory drive currents in XII motoneurons after break-in (Fig. 1A). Normalized (to break-in values) peak currents increased to 190 ± 60% (Fig. 1A, bottom inset) (p < 0.01), reaching peak amplitude in ~15 min (n = 7).
To determine whether endogenous PKA activity affected inspiratory drive currents under our experimental conditions, we recorded with PKI in the patch electrode. Peak endogenous currents decreased 56 ± 13% (Fig. 1B, bottom inset) (p < 0.01) relative to break-in values in a time-dependent manner starting at 4 min after and peaking 10 min after break-in (Fig. 1B) (n = 5).
Because changes in intracellular PKA activity affected inspiratory drive currents, we tested whether changes in phosphatase activity had consistent effects. Inclusion of microcystin, a membrane-impermeable inhibitor of protein phosphatases 1 and 2a, in the patch electrode increased peak endogenous inspiratory drive currents in XII motoneurons (Fig. 1C). Peak currents increased to 170 ± 21% (Fig. 1C, bottom inset) (p < 0.001), reaching peak amplitude 5-30 min after break-in (n = 5).
Effects on exogenous AMPA application
To demonstrate the effect of phosphorylation on AMPA receptor-mediated currents, XII motoneurons were identified as indicated above, and then AMPA (10 µM) was applied exogenously (via micropipette) after bath application of TTX (1 µM). As TTX washed into the recording chamber, rhythmic inspiratory XII nerve activity ceased, as did rhythmic inspiratory drive currents in XII motoneurons. The duration of AMPA injections was adjusted to produce peak inward currents with a shape and peak magnitude similar to endogenous inspiratory currents. Exogenously applied AMPA-induced currents were longer lasting than endogenous inspiratory drive currents, presumably because of the effects of diffusion of pressure-ejected AMPA through the brainstem tissue (Funk et al., 1995
Inclusion of the PKA catalytic subunit in the patch electrode enhanced the peak AMPA-induced current 165 ± 36% (Fig. 2A, bottom inset) (n = 3; p < 0.05). Potentiation of AMPA currents developed slowly over several minutes to a peak value, reaching a maximum 5-16 min after break-in (Fig. 2A).
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Figure 2. Effects of phosphorylation on exogenous AMPA currents. A, Intracellular dialysis of PKA potentiated peak AMPA currents in XII motoneurons. Whole-cell currents produced by focal exogenous AMPA (arrow, 10 µM, 100 msec) in the presence of TTX (1 µM) immediately after break-in followed by 8 and 16 min in an XII motoneuron (Vh =
To determine whether phosphatase inhibition had the same effect on AMPA currents as on endogenous inspiratory drive currents, we performed the above protocol with microcystin (50 µM) in the patch electrode. We observed significantly increased peak whole-cell currents in response to local exogenous AMPA application (Fig. 2B, bottom inset) (202 ± 45%; n = 5; p < 0.001). Maximal effects of microcystin occurred within 15 min of break-in.
Discussion
Our main finding is that a change in PKA activity in XII motoneurons modulates their AMPA receptor-mediated synaptic currents. In XII motoneurons, enhancement of PKA activity (by either increased intracellular PKA or decreased phosphatase activity) increased endogenous synaptic inspiratory drive currents as well as those induced by exogenously applied AMPA; similarly, inhibiting PKA activity depressed these currents.
Changes in the phosphorylation state of ionotropic glutamate receptor subunits (GluRs) contribute to some forms of neuronal plasticity, such as LTP and LTD (Roche et al., 1994
Phosphorylation of AMPA receptors in inspiratory, including XII, motoneurons is postulated to underlie compensatory changes in their excitability in response to physiological challenges. XII motoneurons contribute to the regulation of upper airway resistance, and their failure to produce appropriate output during sleep results in airway collapse. This can cause snoring and OSA (Fogel et al., 2000
We have shown that AMPA currents from functionally active synapses in XII motoneurons are regulated by PKA and protein phosphatases, and that PKA is constitutively active in XII motoneurons in vitro. In in vivo experiments investigating the role of PKA in the neural control of breathing (Lalley et al., 1997
The intracellular balance between protein kinases and phosphatases determines the basal level of phosphorylation (Carvalho et al., 1999
FOOTNOTES Received Sept. 19, 2002; revised Nov. 15, 2002; accepted Nov. 21, 2002.
This work was supported by National Institutes of Health Grant NS24742.
Correspondence should be addressed to Dr. Jack L. Feldman, Department of Neurobiology, David Geffen School of Medicine, University of California Los Angeles, Box 951763, Los Angeles, CA 90095-1763. E-mail: feldman{at}ucla.edu.
References
- Bach KB, Mitchell GS (1996) Hypoxia-induced long-term facilitation of respiratory activity is serotonin dependent. Respir Physiol 104:251-260[Web of Science][Medline].
- Baker-Herman TL, Mitchell GS (2002) Phrenic long-term facilitation requires spinal serotonin receptor activation and protein synthesis. J Neurosci 22:6239-6246
[Abstract/Free Full Text] .- Beattie EC, Stellwagen D, Morishita W, Bresnahan JC, Ha BK, Von Zastrow M, Beattie MS, Malenka RC (2002) Control of synaptic strength by glial TNF
. Science 295:2282-2285
[Abstract/Free Full Text] .- Carvalho AL, Kameyama K, Huganir RL (1999) Characterization of phosphorylation sites on the glutamate receptor 4 subunit of the AMPA receptors. J Neurosci 19:4748-4754
[Abstract/Free Full Text] .- Carvalho AL, Duarte CB, Carvalho AP (2000) Regulation of AMPA receptors by phosphorylation. Neurochem Res 25:1245-1255[Web of Science][Medline].
- Colwell CS, Levine MS (1995) Excitatory synaptic transmission in neostriatal neurons: regulation by cAMP-dependent mechanisms. J Neurosci 15:1704-1713[Abstract].
- Derkach V, Barria A, Soderling TR (1999) Ca2+/calmodulin-kinase II enhances channel conductance of
[Abstract/Free Full Text] .- Figurov A, Boddeke H, Muller D (1993) Enhancement of AMPA-mediated synaptic transmission by the protein phosphatase inhibitor calyculin A in rat hippocampal slices. Eur J Neurosci 5:1035-1041[Web of Science][Medline].
- Fogel RB, Malhotra A, Shea SA, Edwards JK, White DP (2000) Reduced genioglossal activity with upper airway anesthesia in awake patients with OSA. J Appl Physiol 88:1346-1354
[Abstract/Free Full Text] .- Fuller DD, Bach KB, Baker TL, Kinkead R, Mitchell GS (2000) Long term facilitation of phrenic motor output. Respir Physiol 121:135-146[Web of Science][Medline].
- Funk GD, Smith JC, Feldman JL (1993) Generation and transmission of respiratory oscillations in medullary slices: role of excitatory amino acids. J Neurophysiol 70:1497-1515
[Abstract/Free Full Text] .- Funk GD, Smith JC, Feldman JL (1995) Modulation of neural network activity in vitro by cyclothiazide, a drug that blocks desensitization of AMPA receptors. J Neurosci 15:4046-4056[Abstract].
- Ge Q, Feldman JL (1998) AMPA receptor activation and phosphatase inhibition affect neonatal rat respiratory rhythm generation. J Physiol (Lond) 509:255-266
[Abstract/Free Full Text] .- Greengard P, Jen J, Nairn AC, Stevens CF (1991) Enhancement of the glutamate response by cAMP-dependent protein kinase in hippocampal neurons. Science 253:1135-1138
[Abstract/Free Full Text] .- Kameyama K, Lee HK, Bear MF, Huganir RL (1998) Involvement of a postsynaptic protein kinase A substrate in the expression of homosynaptic long-term depression. Neuron 21:1163-1175[Web of Science][Medline].
- Lalley PM, Pierrefiche O, Bischoff AM, Richter DW (1997) cAMP-dependent protein kinase modulates expiratory neurons in vivo. J Neurophysiol 77:1119-1131
[Abstract/Free Full Text] .- Lee HK, Barbarosie M, Kameyama K, Bear MF, Huganir RL (2000) Regulation of distinct AMPA receptor phosphorylation sites during bidirectional synaptic plasticity. Nature 405:955-959[Medline].
- Melis M, Camarini R, Ungless MA, Bonci A (2002) Long-lasting potentiation of GABAergic synapses in dopamine neurons after a single in vivo ethanol exposure. J Neurosci 22:2074-2082
[Abstract/Free Full Text] .- Raymond LA, Blackstone CD, Huganir RL (1993) Phosphorylation and modulation of recombinant GluR6 glutamate receptors by cAMP-dependent protein kinase. Nature 361:637-641[Medline].
- Rekling JC, Funk GD, Bayliss DA, Dong XW, Feldman JL (2000) Synaptic control of motoneuronal excitability. Physiol Rev 80:767-852
[Abstract/Free Full Text] .- Richter DW, Lalley PM, Pierrefiche O, Haji A, Bischoff AM, Wilken B, Hanefeld F (1997) Intracellular signal pathways controlling respiratory neurons. Respir Physiol 110:113-123[Web of Science][Medline].
- Roberson ED, Sweatt JD (1996) Transient activation of cyclic AMP-dependent protein kinase during hippocampal long-term potentiation. J Biol Chem 271:30436-30441
[Abstract/Free Full Text] .- Roche KW, Tingley WG, Huganir RL (1994) Glutamate receptor phosphorylation and synaptic plasticity. Curr Opin Neurobiol 4:383-388[Medline].
- Roche KW, O'Brien RJ, Mammen AL, Bernhardt J, Huganir RL (1996) Characterization of multiple phosphorylation sites on the AMPA receptor GluR1 subunit. Neuron 16:1179-1188[Web of Science][Medline].
- Scanlan MF, Roebuck T, Little PJ, Redman JR, Naughton MT (2000) Effect of moderate alcohol upon obstructive sleep apnoea. Eur Respir J 16:909-913[Abstract].
- Smith JC, Ellenberger HH, Ballanyi K, Richter DW, Feldman JL (1991) Pre-Botzinger complex: a brainstem region that may generate respiratory rhythm in mammals. Science 254:726-729
[Abstract/Free Full Text] .- Snyder GL, Allen PB, Fienberg AA, Valle CG, Huganir RL, Nairn AC, Greengard P (2000) Regulation of phosphorylation of the GluR1 AMPA receptor in the neostriatum by dopamine and psychostimulants in vivo. J Neurosci 20:4480-4488
[Abstract/Free Full Text] .- Soderling TR, Derkach VA (2000) Postsynaptic protein phosphorylation and LTP. Trends Neurosci 23:75-80[Web of Science][Medline].
- Thomas GD, O'Rourke B, Sikkink R, Rusnak F, Marban E, Victor RG (1997) Differential modulation of cortical synaptic activity by calcineurin (phosphatase 2B) versus phosphatases 1 and 2A. Brain Res 749:101-108[Web of Science][Medline].
- Trussell LO, Thio LL, Zorumski CF, Fischbach GD (1988) Rapid desensitization of glutamate receptors in vertebrate central neurons. Proc Natl Acad Sci USA 85:4562-4566
[Free Full Text] .- Wang LY, Salter MW, MacDonald JF (1991) Regulation of kainate receptors by cAMP-dependent protein kinase and phosphatases. Science 253:1132-1135
[Abstract/Free Full Text] .
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