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Previous Article | Next Article
The Journal of Neuroscience, October 15, 1999, 19(20):9107-9116
Two-Stage, Input-Specific Synaptic Maturation in a Nucleus Essential for Vocal Production in the Zebra Finch
Laura L. Stark and David J. Perkel Department of Neuroscience, University of Pennsylvania, Philadelphia, Pennsylvania 19104
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
In most songbirds, vocal learning occurs through two experience-dependent phases, culminating in a reduction of behavioral plasticity called song crystallization. At ends of developmentally plastic periods in other systems, synaptic properties change in a fashion appropriate to limit plasticity. Maturation of glutamatergic synapses often involves a reduction in duration of NMDA receptor (NMDAR)-mediated synaptic responses and a coincident reduction in the contribution of NMDARs to synaptic transmission. We hypothesized that similar changes in the zebra finch song system help limit behavioral plasticity during song development. Nucleus robustus archistriatalis (RA) is a key nucleus in the forebrain song motor pathway and receives glutamatergic input from the motor nucleus HVc. RA also receives glutamatergic input, mediated primarily by NMDARs, from the lateral magnocellular nucleus of the anterior neostriatum, which is part of a circuit essential for learning but not song production. We examined whether synaptic maturation occurs in either input to RA by recording synaptic currents in brain slices prepared from zebra finches of different ages. We find the motor input from HVc to RA uses both AMPA receptors (AMPARs) and NMDARs, and synaptic maturation occurs in two phases: an early reduction in duration of NMDAR-mediated synaptic currents in both inputs, and a later reduction in the NMDAR contribution to synaptic responses in the motor pathway. Although NMDAR kinetics change too early to account for crystallization, the reduction of the relative NMDAR contribution to synaptic transmission could contribute to the onset of crystallization. Thus, synaptic maturation events can be temporally distinct and input-specific and may play different roles in behavioral plasticity.
Key words: NMDA receptor; synaptic maturation; developmental plasticity; neural plasticity; songbird; song learning
INTRODUCTION
Many neural systems undergo periods of activity-dependent developmental plasticity during which key connections are formed, refined, or eliminated (Constantine-Paton et al., 1990
; Katz and Shatz, 1996
We hypothesized that synaptic maturation contributes to neural mechanisms underlying the reduction in behavioral plasticity during song learning in the zebra finch. Most songbirds learn their song during two periods of experience-dependent plasticity lasting several months, after which song becomes highly stereotyped, or "crystallized" (Fig. 1A). A set of interconnected forebrain nuclei, collectively termed the song system, is involved in song learning and production (Brenowitz et al., 1997
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Figure 1. Developmental time line and experimental preparation. A, Developmental time line of song learning showing the four age groups of birds examined in relation to the phases of song learning. B, Schematic drawing of a sagittal view of the male zebra finch brain, depicting a highly simplified song system. There are two major pathways: the motor pathway (HVc, RA, and nXIIts; open nuclei) is necessary for song production; the anterior forebrain pathway (area X, DLM, and lMAN; shaded nuclei) is necessary for song learning but not for song production. C, Schematic drawing of a coronal slice preparation. We stimulated afferent pathways from HVc and lMAN and recorded whole-cell synaptic currents from neurons in nucleus RA. These inputs converge on single RA neurons such that EPSCs from each pathway can be recorded in a single postsynaptic neuron. DLM, Medial portion of the dorsolateral nucleus of the anterior thalamus; HVc, used here as a proper name; lMAN, lateral magnocellular nucleus of the anterior neostriatum; nXIIts, tracheosyringeal portion of the hypoglossal motor nucleus; RA, robust nucleus of the archistriatum; X, area X of the parolfactory lobe.
Preliminary reports of this work have appeared in abstract form (Perkel, 1994
MATERIALS AND METHODS
Animals. A protocol approved by the University of Pennsylvania Institutional Animal Care and Use Committee was used in this study. Zebra finches (Taeniopygia guttata) were obtained either from our own breeding facility (young birds and some adults) or from a local breeder (adult birds only). Birds were housed in cages in two rooms. Each cage contained either a family of birds or a number of adult males. Young male birds were removed to cages with other juveniles ~50 d after hatching [days post-hatch (DPH)], and thus, were sufficiently exposed to the song of their father during the sensory stage of song learning. The four age groups studied were 18-23 DPH, 28-38 DPH, 41-60 DPH, and >100 DPH, corresponding roughly to periods immediately before subsong, at the onset of subsong, at the height of the sensorimotor period, and after song crystallization, respectively (Immelmann, 1969
Preparation of slices. Methods for preparing slices have been described elsewhere (Kubota and Saito, 1991
Electrophysiological recording. We recorded from neurons in nucleus RA using the "blind" whole-cell technique (Blanton et al., 1989
, and electrodes were filled with whole-cell pipette solution, in mM: Cs gluconate 125, HEPES 10, EGTA 10, NaCl 8, MgATP 2, and Na3GTP 0.3, pH 7.3, 290-300 mOsm. Signals were amplified using an Axopatch 1D amplifier (Axon Instruments, Foster City, CA), filtered at 1-3 kHz, digitized at twice the filter frequency with a National Instruments (Austin, TX) digitizing board, and acquired using a custom data acquisition program written in LabView (National Instruments) by M. A. Farries and D. J. Perkel. Series resistance (Rs) was monitored throughout each experiment, and traces in different conditions from the same cell were compared only if there was <20% difference in Rs. Traces shown are an average of 5-20 raw traces.
Using bipolar stainless-steel electrodes (FHC, Bowdoinham, ME), we independently stimulated afferent pathways from HVc and lMAN to elicit EPSCs in RA neurons with a 10 sec interstimulus interval (Fig. 1C). Membrane potential was initially held at
80 mV, and both afferent pathways were stimulated to identify EPSCs. Membrane potential was then held at +50 mV, where both AMPAR- and NMDAR-mediated components could be studied in the region of linearity of the NMDAR current-voltage relationship (Mayer et al., 1984
Analysis. We measured the relative contribution of NMDARs to the EPSC in two ways. In the first method, we obtained the NMDA:AMPA (N:A) ratio by recording a reversed EPSC at +50 mV before and after application of 10 µM CNQX or 50 µM APV. The peak current in the presence of the antagonist provided a measure of one component. The other component was measured as the peak of the current resulting from the subtraction of the EPSC recorded in the presence of the antagonist from the control EPSC. CNQX, in addition to blocking the fast AMPAR-mediated current, also partially reduced the slower NMDA current (31 ± 4% reduction, mean ± SD, data not shown). Before subtraction, the trace recorded in the presence of CNQX was scaled to match the control trace at a point 30 msec after the stimulation artifact, such that the subtraction revealed only the isolated AMPA component. The decay time course of the EPSC recorded in the presence of CNQX was unchanged compared with that of the control EPSC, supporting our criteria for minimizing the occurrence of polysynaptic inputs in our data set. In the second method, we obtained a measure of the two components independent of pharmacology. Taking advantage of the different kinetics of the two components, we measured the ratio of the late (NMDA) component to the early (AMPA) component, the Late:Early ratio (Hestrin et al., 1990a
To measure decay kinetics of the NMDAR-mediated synaptic current, we isolated that synaptic component using CNQX, which had no effect on the decay time course (data not shown). Two methods were used to quantify the NMDAR decay kinetics: e-fold decay time and double exponential analysis. e-fold decay was measured as the time (in milliseconds) from peak to peak × (1/e). To measure the fast and slow components of the NMDAR-mediated EPSC, we fitted the trace with a double exponential decay function: Y(t) = amp1 × e(-K1 × t) + amp2 × e(-K2 × t) + asymptote, using the iterative CurveFit function (IgorPro 3.12; WaveMetrics, Lake Oswego, OR), which minimized the least-squares difference between the averaged trace and the double exponential function. The asymptote was constrained to the baseline value. We then determined the decay time constants (in milliseconds) of the fast (
f = 1/K1) and slow (
Unless otherwise specified, one-way ANOVA was used to test for a developmental change in a given measurement. Subsequently, Newman-Keuls tests were used for unplanned pairwise comparisons between groups (Prism 2.01; Graphpad Software, San Diego, CA). Unless otherwise noted, data are presented as mean ± SD.
RESULTS
lMAN-RA and HVc-RA synapses use different complements of glutamate receptor subtype
We recorded reversed synaptic currents from RA neurons at a holding potential of +50 mV by stimulating the afferent pathways from HVc (HVc-RA EPSCs) and from lMAN (lMAN-RA EPSCs). The NMDAR- and AMPAR-mediated components were studied using CNQX, an antagonist of AMPARs and/or APV, an antagonist of NMDARs. We found that HVc-RA synapses use both NMDARs and AMPARs, whereas lMAN-RA synapses use NMDARs almost exclusively (Fig. 2). Application of 50 µM APV blocked the NMDA component of the HVc-RA EPSC, revealing a substantial AMPAR-mediated component with a rapid onset and decay (Fig. 2A). In contrast, APV blocked nearly all of the lMAN-RA EPSC, revealing only a negligible AMPA component (Fig. 2B). Subsequent addition of 10 µM CNQX eliminated the remaining synaptic current (Fig. 2A,B). In separate experiments, antagonists were applied in the reverse order to confirm this effect and to illustrate the shape of the NMDAR-mediated component (Fig. 2C,D). Application of 10 µM CNQX blocked the AMPA component of the HVc-RA EPSC, revealing a substantial NMDA component with a slow time course of onset and decay (Fig. 2C). However, CNQX had minimal effect on the lMAN-RA EPSC (Fig. 2D). Subsequent addition of APV eliminated the remaining synaptic current in both pathways (Fig. 2C,D).
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Figure 2. EPSCs from HVc and lMAN inputs are mediated by different complements of glutamate receptor subtype. EPSCs elicited by HVc afferent stimulation (A, C) are mediated by both AMPARs and NMDARs, whereas EPSCs elicited by lMAN afferent stimulation (B, D) are mediated almost exclusively by NMDARs. Each panel shows three EPSCs (each an average of 5-20 traces), overlaid and aligned at the time of stimulation. Some stimulus artifacts have been clipped for clarity. APV blocked the NMDA component, revealing a substantial AMPA component in the HVc-RA EPSC (A), and a negligible AMPA component in the lMAN-RA EPSC (B); AMPA components were subsequently blocked by CNQX. Initial application of CNQX blocked the AMPA component in the HVc-RA EPSC, revealing a substantial NMDA component (C), but had minimal effect on the lMAN-RA EPSC (D); NMDA components in both pathways were subsequently blocked by APV. EPSCs in A and B are from a single neuron from a 43 DPH bird; EPSCs in C are from an adult bird; EPSCs in D are from a 42 DPH bird.
To quantify the contribution of NMDARs to the synaptic current, we calculated the ratio of peak currents mediated by NMDARs and AMPARs (N:A ratio; see Materials and Methods). The median N:A ratio for HVc-RA EPSCs was >1 (median, 1.44; range, 0.57-3.88; n = 19), indicating a substantial NMDAR contribution in the HVc input. N:A ratios for lMAN-RA EPSCs were much larger (median, 10.27), and the AMPA component was often indistinguishable from background, resulting in an apparently non-normal distribution of N:A ratios with a large range (2.61-98.27; n = 23). Figure 3 shows that HVc and lMAN N:A ratios, combining all age groups, are significantly different (Mann-Whitney U test; U = 7.00; p < 0.0001). These results confirm previous reports that lMAN-RA synapses are mediated almost exclusively by NMDARs (Kubota and Saito, 1991
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Figure 3. Comparison of NMDA:AMPA ratio between HVc-RA and lMAN-RA EPSCs. N:A ratio values (and median plus interquartile range) for all ages examined, plotted on a log scale. The dotted line indicates a 1:1 ratio. In this and subsequent figures, each individual symbol represents data from one cell. Median N:A ratio for lMAN-RA EPSCs is approximately tenfold higher than that for HVc-RA EPSCs, illustrating that lMAN-RA EPSCs are mediated predominantly by NMDARs, whereas HVc-RA EPSCs are mediated by both NMDARs and AMPARs.
The contribution of NMDARs to HVc-RA EPSCs decreases during development
The contribution of the NMDAR to the dual-component EPSC decreases during development in many systems (Fox et al., 1989
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Figure 4. Developmental reduction in NMDAR contribution to total synaptic current. A1, Scatterplot of NMDA:AMPA ratio versus age for HVc-RA EPSCs. In this and subsequent figures, cells from adult birds are plotted at 100 DPH. A2, Mean N:A ratio values (± SD) for HVc-RA EPSCs. The N:A ratio decreased during development, but post hoc tests did not identify differences between groups. B1, Scatterplot of Late:Early ratio, an independent measure of the contribution of NMDAR to the total EPSC, versus age. B2, Mean Late:Early ratio values (± SD) for HVc-RA EPSCs. Late:Early ratio also decreased during development. Post hoc tests revealed that the decrease in Late:Early ratio occurred between the juvenile and adult stages, but inspection of the scatterplot (B1) suggests that the decrease may occur during the juvenile stage. See Table 1 for statistics. NS, Not significant.
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Table 1. Statistical analysis of synaptic maturation of HVc and lMAN inputs to RA N:A ratio and Late:Early ratios from nestlings are not included in Figure 4 or in statistical analyses for two reasons. First, the frequency of obtaining an acceptable HVc-RA EPSC in nestlings was very low (3 of 42 attempts; seven other inputs were polysynaptic and were not used), and only one of these yielded N:A data (N:A, 0.73). In all cells, HVc afferents were stimulated while holding membrane potential at
Decay kinetics of lMAN-RA and HVc-RA EPSCs decrease early in song development
In addition to developmental changes in N:A ratio, the decay kinetics of NMDAR-mediated synaptic currents change during development (Carmignoto and Vicini, 1992
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Figure 5. Example traces showing a developmental decrease in duration of NMDAR-mediated EPSCs. Normalized EPSCs from different ages for both lMAN (A) and HVc (B) inputs to RA. The duration of the isolated NMDAR-mediated current decreased dramatically between the nestling stage (20 DPH in A, 23 DPH in B) and the fledgling stage (34 DPH in A, 28 DPH in B). There was no further change between fledglings and adults. Juvenile examples are omitted for clarity, but the time course resembles that of the fledgling and adult traces.
To quantify the decay time course of NMDAR-mediated currents, we measured e-fold decay time and fitted currents with a double exponential decay function. Both lMAN-RA and HVc-RA EPSCs exhibited a significant developmental reduction in e-fold decay time (Table 1, Fig. 6A1, B1). Post hoc tests showed that e-fold decay time for the nestling group was significantly different from that for each of the other three groups, but that fledglings, juveniles, and adults were not significantly different from one another (Table 1, Fig. 6A2, B2). Thus e-fold decay time decreased significantly between the nestling and fledgling groups and then remained at the same level throughout the remainder of development.
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Figure 6. e-fold decay time decreases early in song development. A1, Scatterplot of e-fold decay times versus age for lMAN-RA EPSCs. For this and subsequent figures, filled symbols are from males, open symbols are from females or birds of unknown sex (see Materials and Methods). A2, Mean e-fold decay time (± SD) for lMAN-RA EPSCs. B1, Scatter plot of e-fold decay times versus age for HVc-RA EPSCs. B2, Mean e-fold decay time (± SD) for HVc-RA EPSCs. For both inputs, nestlings had significantly longer e-fold decay times than any of the other age groups (***p < 0.001, comparing nestlings with each of the other groups). There were no significant differences among fledglings, juveniles, and adults, indicating that e-fold decay time stabilized by the fledgling stage. See Table 1 for statistics.
NMDAR-mediated synaptic currents in other systems are composed of both a fast and a slow component, for which the decay time constants are determined by the subunit composition of the receptor (Hestrin et al., 1990b
We performed a double exponential analysis on lMAN-RA and HVc-RA EPSCs to test the hypothesis that a decrease in % slow was the critical factor in decreasing the duration of the synaptic currents. Unexpectedly, the most dramatic effect was a decrease in
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Figure 7. Decay time constants decrease early in song development. Scatterplots of three variables (
Overall, for both e-fold decay and double exponential analyses, we found that the decay kinetics for both lMAN and HVc inputs to RA decreased between the nestling and fledgling age groups, and that there was no difference in any of the measures among the three older groups. One possible confounding effect was that birds in the nestling age group do not exhibit secondary sexual characteristics. For the HVc-RA EPSCs, both data points in the nestling group were from confirmed male birds. However, not all birds contributing to the nestling lMAN data were male; four birds were male, four birds were female, and two birds were of unconfirmed sex. t tests comparing confirmed males versus females plus birds of unknown sex indicated that there was no difference between these two groups (p > 0.05 in all cases, data not shown), so all data were pooled, and we did not consider the sex difference to confound the data.
Finally, inspection of the overlaid traces in Figure 5 suggests that the rise time of NMDAR-mediated EPSCs might also change with development. One-way ANOVAs showed that there was no developmental change in rise time of lMAN-RA EPSCs, but there was a change for HVc-RA EPSCs (Table 1). As for previous analyses of kinetic properties, subsequent post hoc analyses of the rise times for HVc-RA EPSCs indicated that the difference lies between the nestling and fledgling stages and that there is no difference among the three older age groups.
DISCUSSION
Here we confirm previous findings that the lMAN input to RA is mediated almost exclusively by NMDARs (Kubota and Saito, 1991
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Figure 8. Schematic representation of two-stage, input-specific synaptic maturation in RA neurons. A, In nestlings, NMDARs with slow decay kinetics (filled ovals) mediate synaptic transmission at lMAN-RA synapses. At this age, HVc inputs are rare and are not shown here; however, the few NMDAR-mediated currents we have recorded had slow decay times. B, At the fledgling and juvenile stages, NMDARs mediating both HVc-RA and lMAN-RA EPSCs have fast decay kinetics (open ovals). HVc inputs are mediated by both NMDARs and AMPARs (filled rectangles) with an ~2:1 ratio. C, By adulthood, the relative contributions of NMDARs and AMPARs have decreased to an ~1:1 ratio, and the decay kinetics of NMDARs remain fast in both input pathways. The symbol key, inset in A, applies to A-C. D, Summary of our observations, depicting the spatial and temporal dissociation of two forms of synaptic maturation in nucleus RA.
Differential synaptic maturation of two converging inputs
Studies in mammals and amphibians have identified two major functional changes in glutamatergic synaptic transmission that occur hand in hand: a decrease in the N:A ratio and a shortening of NMDAR-mediated EPSCs (Crair and Malenka, 1995
Our results are summarized in Figure 8D, illustrating the spatial and temporal dissociation of the two forms of synaptic maturation. That these two processes occur in the same population of postsynaptic neurons suggests that they are subject to differential control. The innervation of RA by HVc inputs and the ensuing arrival of motor signals, may trigger the change in NMDAR kinetics in the postsynaptic cells. Alternatively, some other signal could trigger both the changes in kinetics and the massive innervation of RA by HVc axons. The change in relative contribution of NMDARs to synaptic transmission occurs at least 3 weeks later, well after HVc has fully innervated RA (Akutagawa and Konishi, 1994
Differential glutamate receptor complements mediating inputs to RA neurons
Three previous studies using sharp electrode intracellular recording under current-clamp conditions reported that the input from lMAN to RA was almost entirely blocked by APV and was only slightly reduced by CNQX (Kubota and Saito, 1991
In addition to their important role in triggering neural plasticity, NMDARs also contribute to basic synaptic transmission (Salt, 1986
RA projection neurons make collateral excitatory synapses onto their neighbors, which, like HVc-RA synapses, are mediated by both AMPARs and NMDARs (Perkel, 1995
Possible mechanisms of the two stages of synaptic maturation
The duration of mammalian NMDAR-mediated EPSCs is governed by the glutamate affinity of the receptor (Lester et al., 1990
In thalamic inputs from the medial portion of the dorsolateral nucleus of the anterior thalamus (DLM) to zebra finch lMAN, the duration of NMDAR-mediated EPSCs decreases between ~30 and 40 DPH (Livingston and Mooney, 1997
Boettiger and Doupe (1998)
The molecular processes underlying maturation of NMDAR decay kinetics at DLM-lMAN and lMAN-RA synapses are likely different. Developmental changes in binding of the broad-spectrum NMDAR antagonist MK-801 and the subunit-specific ligand ifenprodil suggest there is developmental regulation of NMDAR density and subunit expression within lMAN (Aamodt et al., 1994
Implications for song learning
We have begun to address possible neural mechanisms of song learning by examining developmental regulation of NMDAR-mediated synaptic transmission in nucleus RA of the zebra finch, in relation to different phases of song learning. We originally predicted that in RA, synaptic maturation (both forms) would occur concomitantly with song crystallization. We found that only one form of synaptic maturation occurs during the sensorimotor learning phase. Whether this represents the unfolding of a developmental program or contributes in some way to changes in song learning ability remains unknown. Nonetheless, during the sensorimotor phase and into adulthood, NMDAR kinetic properties do not change. Our observations thus argue against shortening of NMDAR time course in RA as a mechanism for crystallization.
FOOTNOTES Received June 17, 1999; revised Aug. 3, 1999; accepted Aug. 3, 1999.
This work was supported by National Institutes of Health Grants F32 DC00330 to L.L.S. and R01 MH56646 to D.J.P. We thank Jessica Cardin, Long Ding, Michael Farries, Minmin Luo, and Paul Nealen for helpful discussions and comments on an earlier version of this manuscript.
Correspondence should be addressed to David J. Perkel, 215 Stemmler Hall, Department of Neuroscience, University of Pennsylvania, Philadelphia, PA 19104-6074.
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