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The Journal of Neuroscience, February 1, 2002, 22(3):740-747
Cell Type- and Subcellular Position-Dependent Summation of Unitary Postsynaptic Potentials in Neocortical Neurons
Gábor Tamás1, 2, János Szabadics1, and Peter Somogyi2 1 Department of Comparative Physiology, University of Szeged, Szeged H-6726, Hungary, and 2 Medical Research Council Anatomical Neuropharmacology Unit, Department of Pharmacology, University of Oxford, Oxford, OX1 3TH, United Kingdom
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Theoretical studies predict that the modes of integration of coincident inputs depend on their location and timing. To test these models experimentally, we simultaneously recorded from three neocortical neurons in vitro and investigated the effect of the subcellular position of two convergent inputs on the response summation in the common postsynaptic cell. When scattered over the somatodendritic surface, combination of two coincident excitatory or inhibitory synaptic potentials summed linearly in layer 2/3 pyramidal cells, as well as in GABAergic interneurons. Slightly sublinear summation with connection specific kinetics was observed when convergent inputs targeted closely placed sites on the postsynaptic cell. The degree of linearity of summation also depended on the type of connection, the relative timing of inputs, and the activation state of Ih. The results suggest that, when few inputs are active, the majority of afferent permutations undergo linear integration, maintaining the importance of individual inputs. However, compartment- and connection-specific nonlinear interactions between synapses located close to each other could increase the computational power of individual neurons in a cell type-specific manner.
Key words: cerebral cortex; integration; IPSP; EPSP; interneuron; pyramidal cell
INTRODUCTION
The rules of synaptic summation are thought to depend on the dendritic geometry of the postsynaptic cell (Zador et al., 1995
; Mainen et al., 1996
MATERIALS AND METHODS
Electrophysiology. Young (postnatal days 17-30) Wistar rats were anesthetized by the intraperitoneal injection of ketamine (30 mg/kg) and xylazine (10 mg/kg), and, after decapitation, coronal slices (350-µm-thick) were prepared from their somatosensory cortex. Slices were incubated at room temperature for 1 hr in a solution composed of (in mM): 130 NaCl, 3.5 KCl, 1 NaH2PO4, 24 NaHCO3, 1 CaCl, 3 MgSO4, and 10 (+)D-glucose, saturated with 95% O2 and 5% CO2. The solution used during recordings differed only in that it contained 3 mM CaCl2 and 1.5 mM MgSO4. Micropipettes (5-7 M
) were filled with (in mM): 126 K-gluconate, 4 KCl, 4 ATP-Mg, 0.3 GTP-NA2, 10 HEPES, 10 kreatin-phosphate, and 8 biocytin, pH 7.25 (300 mOsm). Somatic whole-cell recordings were obtained at ~36°C from concomitantly recorded triplets and quadruplets of interneurons and pyramidal cells visualized in layers 2/3 by infrared differential interference contrast videomicroscopy [Zeiss (Oberkochen, Germany) Axioskop microscope, Hamamatsu (Hamamatsu City, Japan) CCD camera, Luigs & Neumann (Ratingen, Germany) Infrapatch set-up, and two Heka Elektronik (Lambrecht/Pfalz, Germany) EPC 9 double-patch-clamp amplifiers]. Signals were filtered at 8 kHz, digitized at 16 kHz, and analyzed with PULSE software (Heka Elektronik). In all, 237 simultaneous triple and 316 quadruple recordings yielded 258 unitary connections interconnecting fast-spiking (FS), bitufted (BT), and pyramidal cells in the studied directions. In 28 cases, convergent afferents to a common postsynaptic neuron were recorded and are reported here. During stimulation, presynaptic cells were stimulated with brief (2 msec) suprathreshold pulses delivered at
5 sec intervals to minimize intertrial variability. Presynaptic cells were stimulated in cycles containing single presynaptic cell activations and synchronous and asynchronous dual presynaptic activation. For synchronous presynaptic activation, action potentials were timed to synchronize maximal unitary postsynaptic current amplitudes measured before the experiments testing convergence. Membrane potentials were corrected for junction potentials. Voltage-clamp recordings were excluded from analysis when series resistance was higher than 25 M
20 to 0 msec before the onset of current injections into the presynaptic neuron. The amplitude of postsynaptic event was defined as the difference between the peak amplitude and the baseline value measured 0-20 msec before presynaptic activation. Data for analysis of summation were used only from epochs in which the postsynaptic response remained stationary, i.e., the mean amplitude of 10 consecutive events remained within ±10% of the mean of the first 10 events of the epoch. The difference between the algebraic sums of single input responses and the recorded summed response was calculated during postsynaptic responses and expressed as a percentage of the maximal amplitude of the calculated response at the given time point. The resulting waveform is used as a measure of the degree of linearity over time.
Histology. Visualization of biocytin was performed as described previously (Tamás et al., 2000
Data are presented as mean ± SD; Statistica for Windows software package was used for statistical analysis (StatSoft Inc., Tulsa, OK). The significance for all comparisons was set at p < 0.05.
RESULTS
Of several hundred multiple recordings made, the physiological analysis of 28 triple cell recordings involving convergent inputs onto the same postsynaptic cell in layers 2/3 of somatosensory cortex was performed in detail. Of these, satisfactory intracellular labeling of all three cells permitted the unequivocal tracing of afferents back to the parent somata in 12 cases. Pairs of presynaptic pyramidal or FS cells were activated using a cyclic stimulation paradigm (Fig. 1b) (see Fig. 4b) that evoked simultaneous presynaptic action potentials with a relative peak to peak difference of 0.14 ± 0.12 msec. Postsynaptic cells receiving two convergent inputs represented pyramidal neurons, FS and BT cells (McCormick et al., 1985
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Figure 1. Linear summation of convergent excitatory inputs. a-g, Summation of convergent EPSPs in a layer 3 FS cell. a, Firing pattern of the presynaptic pyramidal cells (red and blue) and the postsynaptic FS cell (black). b, Current-clamp recordings of summation. Repeated and cyclic activation of the presynaptic cells (1, red pyramid alone; 2, blue pyramid alone; 1 and 2, both cells together) resulted in unitary EPSPs (black 1, black 2) and compound responses (black 1 and 2) in the postsynaptic interneuron held at
Summation of convergent EPSPs and EPSCs
Integration of convergent unitary EPSPs evoked by local layer 2/3 pyramidal neurons was tested in nine FS cells, four BT neurons, and two pyramidal cells (Figs. 1-3). Based on the linearity of summation between synchronous inputs, pyramid to FS connections could be clearly divided into two groups. Unitary EPSPs summed linearly in five FS cells, but moderately sublinear summation was detected in four postsynaptic FS neurons. In the linearly summating group of cells, amplitudes of the converging smaller and bigger unitary EPSPs were 0.99 ± 0.77 and 2.11 ± 1.84 mV measured at
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Figure 2. Sublinear summation of convergent EPSPs in FS cells. a, Repeated and cyclic activation of the presynaptic cells (top; 1, red pyramid alone; 2, blue pyramid alone; 1 and 2, both cells together) elicited unitary EPSPs (middle; black 1, black 2) and compound responses (black 1 and 2) in the postsynaptic FS cell held at
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Figure 3. Linear summation of convergent, facilitatory EPSPs in a layer 3 bitufted cell. a, Firing pattern of the presynaptic pyramidal cells (red and blue) and the postsynaptic BT cell (black). b, Repeated activation of the presynaptic pyramidal cells with paired pulses (1, red pyramid alone; 2, blue pyramid alone; 1 and 2, both cells together) resulted in unitary EPSPs (black 1, black 2) and compound responses (black 1 and 2) in the postsynaptic BT cell held at
In two FS cells, similar experimental paradigms were applied holding the postsynaptic cells in voltage-clamp mode (Figs. 1c, 2b). Although measurements in current-clamp mode indicated linear (Fig. 1b) or sublinear (Fig. 2a) integration, summation of postsynaptic currents was close to linear in both cases, because the amplitudes of recorded composite EPSCs were 99.6 and 97.5% of the algebraic sums of individually evoked EPSCs (Figs. 1c, 2b).
To investigate the effect of the relative timing of two EPSPs on their summation characteristics in FS neurons, we tested how asynchronous EPSPs interact by eliciting the smaller unitary responses (0.66 ± 0.38 mV) 5 msec after the bigger EPSPs (1.46 ± 0.52 mV) in two triplets showing linear and in two triplets showing sublinear summation of synchronous inputs. Asynchronous activation produced linear summation (100.7 ± 0.9%) in all four cases, because recorded compound events and calculated sums of unitary PSPs were similar in amplitude (1.41 ± 0.38 and 1.40 ± 0.39 mV), as measured at the peak of the single smaller EPSP (Fig. 2c).
Summation characteristics might depend on the amplitude of inputs. Therefore, we examined the degree of linearity as a function of EPSP amplitude measured as the maximal amplitude of the algebraic sums of individual EPSPs and found no correlation in pyramid to FS cell triplets (n = 9; Spearman correlation; r = 0.13; p > 0.5). Moreover, we tested the summation of EPSPs on BT cells (n = 4), because pyramidal inputs to these cells show relatively strong paired-pulse facilitation (Markram et al., 1998
Structural analysis of the basis of convergent EPSPs showing linear integration properties was performed in four triplets with two FS cells and two BT cells receiving the pyramidal inputs. On average, unitary innervation was mediated by 2.0 ± 0.8 and 2.8 ± 1.7 predicted contact sites by the axons evoking the smaller and bigger unitary EPSPs, respectively. Measured from the soma, postsynaptic cells were innervated at distances of 79 ± 35 and 76 ± 23 µm by the weaker and stronger inputs, respectively. The two sets of afferents contacted different dendritic segments in all cases, and the contact sites made by the two presynaptic pyramids were relatively distant from each other on the postsynaptic cell (146 ± 42 µm) (Fig. 1e,f). Electron microscopic testing of all suspected contact sites confirmed light microscopic predictions as being synaptic junctions in the triplet presented in Figure 1a-g. Anatomical analysis of pyramid to FS triplets, which showed sublinear summation, could be performed in two cases. In contrast to distant input sites in triplets producing linear EPSP summation, boutons evoking EPSPs summating sublinearly were relatively close to one another. Light microscopic evaluation of the first triplet indicated five and two contact sites for the two inputs with an average distance of 55 ± 21 µm (n = 10), as measured along the dendrites between all individual predicted synapses of distinct origin. Both presynaptic cells made two contacts on dendritic branches originating from the same stem, and the nearest two synapses made by the two presynaptic axons were 7 µm apart. Analysis of the second triplet revealed that the two inputs targeted the same dendritic segment of the postsynaptic FS cell (Fig. 2d). The average distance of the two inputs was 14 ± 3 µm (n = 2), as proved by electron microscopy.
Summation of convergent IPSPs and IPSCs
The data derived from EPSP-EPSP interactions indicated that neighboring input positions might result in sublinear summation. Extensive testing of this hypothesis requires input combinations reliably targeting the same postsynaptic domain. Cortical basket cells show FS firing pattern; they selectively target the perisomatic region of postsynaptic cells and frequently innervate pyramidal cells in their vicinity (Somogyi et al., 1998
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Figure 4. Summation of convergent IPSPs evoked by FS cells in pyramidal cells. a-h, Coaligned GABAergic inputs to a layer 3 pyramidal cell. a, Firing pattern of the presynaptic FS cells (red and blue) and the postsynaptic pyramidal cell (black). b, Current-clamp recordings of the interaction. Activation of the presynaptic cells (1, red FS cell alone; 2, blue FS cell alone; 1 and 2, both cells together) resulted in unitary IPSPs (black 1, black 2) and compound responses (black 1 and 2) in the postsynaptic interneuron held at
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Figure 5. Temporal and pharmacological properties of IPSP summation in convergent FS cell to pyramidal cell connections. a, b, Synchronous (a) or asynchronous (b) activation of the presynaptic cells (top; FS cell 1 alone, FS cell 2 alone; 1 and 2, both cells together) elicited unitary IPSPs (middle; black 1, black 2) and compound responses (black 1 and 2') in the postsynaptic pyramidal cell held at
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Figure 6. The degree of linearity in the summation of PSPs is connection and subcellular position dependent. a, Average time course of the degree of linearity in the summation of converging unitary EPSP-EPSP (epsp+epsp; n = 4) and IPSP-IPSP (ipsp+ipsp; n = 8; n = 6 in ZD7288) connections, which showed sublinear summation. Gray areas indicate SDs. b, Amplitude normalization of traces shown in a shows that, in EPSP-EPSP in FS cell connections, sublinearity is temporally restricted relative to IPSP-IPSP in pyramid connections. c, Kinetics of linearity relative to corresponding unitary synaptic currents and potentials in sublinearly summating unitary connections (see Results). d, e, Summation of unitary postsynaptic potentials is position dependent. The average distance between two sets of afferent synapses (d) and the distance between nearest neighboring synapses of the two converging axons (e) measured along the postsynaptic soma and dendrites correlates with the degree of linearity in postsynaptic response summation. Dots in the symbols indicate cases in which the site of synaptic junctions was established by electron microscopy; in the remaining cases, distances were mapped by light microscopy.
We tested how asynchronous IPSPs interact by eliciting the smaller unitary responses (0.82 ± 0.48 mV) 5 msec after the bigger IPSPs (2.05 ± 1.64 mV) in two triplets showing linear and in three triplets showing sublinear summation of synchronous inputs (Fig. 5). Asynchronous activation did not change the properties of summation compared with synchronous timing of inputs; the difference in the degree of linearity of the peak response between synchronous and corresponding asynchronous input combinations was 0.6 ± 4.2% (Fig. 5a,b). We also tested synchronous input summation in five pyramidal cells holding the postsynaptic cells in voltage-clamp mode (Fig. 4d). Although, for these connections, the measurements in current-clamp mode indicated either linear (n = 2) or sublinear (n = 3) (Fig. 4b) integration, summation of postsynaptic currents was close to linear in all five cases, because the amplitudes of recorded composite IPSCs were 97.0 ± 2.0% of the algebraic sums of individually evoked IPSCs (Fig. 4d).
Summation properties are likely to depend on voltage-gated conductances, and Ih is thought to be the most prominent current activated by IPSPs in pyramidal cells. Therefore, after completing some of the protocols detailed above in normal extracellular solution, we continued some experiments (n = 6) in the presence of the channel blocker ZD7288 (40 µM) (Fig. 5). The application of ZD7288 increased the input resistance of pyramidal cells by 38 ± 19% and the amplitude and decay time constant of unitary IPSPs to 133 ± 25 and 137 ± 24% of the control, respectively (all three, p < 0.05; Wilcoxon test). When synchronously activating the smaller and bigger IPSPs (1.02 ± 0.84 and 3.19 ± 2.65 mV) in the presence of ZD7288, all six triplets showed sublinear summation, although control measurements indicated three linearly and three sublinearly summating input combinations (99.7 ± 0.5 and 93.6 ± 2.1%, respectively). Overall, ZD7288 significantly increased sublinearity from 96.7 ± 3.5 to 90.4 ± 3.9% (n = 6; p < 0.05; Wilcoxon test). The time course of the degree of linearity and IPSPs were different (Fig. 5c), as shown by the difference in the decay time constants (IPSP, 87.9 ± 9.3 msec vs linearity, 53.5 ± 12.3 msec; p < 0.05; Wilcoxon test). Asynchronous activation of the convergent inputs (n = 6) in the presence of ZD7288 changed the degree of linearity of the peak response from 90.4 ± 3.9 to 95.9 ± 6.2% (p < 0.05; Wilcoxon test) (Fig. 5d), resulting in linearization of three input combinations.
Anatomical analysis of the connections providing convergent IPSPs with sublinear integration properties could be performed in four triplets (Fig. 4e-h). All eight presynaptic FS cells innervated pyramidal cells on or relatively close to the soma. Predicted and/or electron microscopically verified synapses were 20 ± 21 µm from the postsynaptic somata. The average distance between the two sets of contact sites was 41 ± 13 µm, and the closest synapses-contacts originating from two converging presynaptic cells were 12 ± 14 µm apart measured along the postsynaptic dendrites or estimated on the soma. In five measurements of basket cell input to pyramidal cells, light microscopic estimates of somatic synapses cannot account for those that are obscured by the soma; therefore, these estimates are less accurate. Electron microscopic serial section analysis of all suspected contact sites in one triplet showed coalignment of inputs on the soma and proximal dendrites of the postsynaptic cell (Fig. 4e-h). One of the presynaptic FS cells in the somatic cotermination case established synapses (n = 6) exclusively on the cell body, whereas the other presynaptic FS cell targeted the cell body by four synapses and the proximal apical dendrite by three synapses. The distance between the synapses formed by the two presynaptic cells was, on average, 23 ± 22 µm. From the linearly summating triplets, two triplets could be analyzed anatomically. Light microscopic estimates indicated that the postsynaptic pyramidal cells were innervated by two and two contact sites by the cells evoking the smaller IPSPs and 14 and five presumed synapses by the bigger unitary IPSPs, respectively. The four presynaptic cells innervated the postsynaptic cells at an average distance of 32 ± 14 µm from the soma. The mean dendritic distance of the convergent sets of afferents was 59 ± 16 and 73 ± 24 µm from each other, and the nearest neighbors of distinct sources were 42 and 39 µm distant.
Synapse location dependence of the degree of linearity in input summation
Overall, when comparing the time course of the degree of linearity in converging EPSPs on FS cells and converging perisomatic IPSPs on pyramidal cells showing sublinear summation, both the 10-90% rise time and decay time constant are faster in FS cells than in pyramidal neurons (p < 0.01; Mann-Whitney U test). This indicates that the temporal dynamics of the degree of linearity are connection and/or cell type specific. However, the combined analysis also revealed that EPSP-EPSP and IPSP-IPSP interactions summate similarly, depending on the spatial arrangement of inputs on the postsynaptic neuron (Fig. 6d,e). The average somatodendritic distance of the two sets of afferents and the distance between nearest neighboring synapses made by the two different converging cells correlated with the linearity of input summation (r = 0.81 and r = 0.85; p < 0.001; Spearman correlation).
DISCUSSION
Our results provide direct experimental evidence that the summation of two convergent unitary inputs follows linear or close to linear summation in cortical neurons in vitro. This suggests that, when a small number of afferents are simultaneously active, linear or moderately sublinear summation dominates the integration of inputs as detected at the soma. Taking cortical interneurons, their total dendritic lengths were estimated as between 2500 and 12,000 µm per neuron and synaptic density as between 150 and 500 synapses per 100 µm dendritic length (Gulyas et al., 1999
Electron microscopic determination of the sites of synaptic junctions provided by the functionally tested converging afferents revealed that the distance between distinct simultaneously active inputs influences the degree of linearity of summation. Supporting predictions made by cable theory (Jack et al., 1975
Nonlinear interactions may increase the computational power of neurons (Koch et al., 1983
In pyramidal neurons, Ih is likely to be one of the conductances involved in shaping integration properties. Moderate activation of Ih by preceding unitary IPSPs might explain that asynchronous perisomatic IPSPs also showed sublinear summation characteristics. The degree of linearity was correlated with the amplitude of convergent IPSPs; therefore, the increased sublinearity during Ih blockade could result from the greater drop in driving force produced by the larger IPSPs. However, additional experiments are needed to explain the observation that synchronous and asynchronous IPSPs summed similarly in control conditions but desynchronization reduced sublinearity during ZD7288 application. Our results also indicate that Ih tends to linearize the summation of IPSPs arriving proximally. The scenario for dendritic IPSPs might be different, because Ih and other conductances, which might shape integration properties, are preferentially expressed on distal dendrites (Hoffman et al., 1997
The relative weight of linear and nonlinear interactions of inputs in single neurons could be influenced also by the timing of convergent inputs. Although we have not been able to test the wide range of spatiotemporal parameters of previous simulations examining the time course of nonlinear interactions (Koch et al., 1983
FOOTNOTES Received Sept. 5, 2001; revised Oct. 18, 2001; accepted Oct. 22, 2001.
This work was supported by the James S. McDonnell Foundation (Eastern European Science Institute Grant 97-39), the Wellcome Trust, and the Hungarian Scientific Research Fund (Grant D32815). G.T. was a János Bolyai scholar during part of this project. We thank Dr. N. Kogo for help in instrumentation and scientific advice, Dr. L. Marton for calculating theoretical limits for linear input summation, Dr. Z. Nusser for helpful discussions, Drs. I. Mody, G. Buzsáki, and C. Stricker for comments on an earlier version of this manuscript, and A. Lorincz and E. Toth for technical help.
Correspondence should be addressed to Dr. Gábor Tamás, University of Szeged, Department of Comparative Physiology, Középfasor 52, Szeged, H-6726, Hungary. E-mail: gtamas{at}sol.cc.u-szeged.hu.
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