Reversible Disorganization of the Locomotor Pattern after Neonatal Spinal Cord Transection in the Rat

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The Journal of Neuroscience, March 1, 2003, 23(5):1924

Reversible Disorganization of the Locomotor Pattern after Neonatal Spinal Cord Transection in the Rat
Jean-Chrétien Norreel^*, Jean-François Pflieger^*, Edouard Pearlstein, Juliette Simeoni-Alias, François Clarac, and Laurent Vinay
Développement et Pathologie du Mouvement, Centre National de la Recherche Scientifique, F-13402 Marseille Cedex 20, France

  ABSTRACT

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

The central pattern generators (CPGs) for locomotion, located in the lumbar spinal cord, are functional at birth in the rat.Their maturation occurs during the last few days preceding birth,a period during which the first projections from the brainstemstart to reach the lumbar enlargement of the spinal cord. Thegoal of the present study was to investigate the effect of suppressinginputs from supraspinal structures on the CPGs, shortly aftertheir formation. The spinal cord was transected at the thoraciclevel at birth [postnatal day 0 (P0)]. We examined during thefirst postnatal week the capacity of the CPGs to produce rhythmicmotor activity in two complementary experimental conditions. Leftand right ankle extensor muscles were recorded in vivo duringairstepping, and lumbar ventral roots were recorded in vitro duringpharmacologically evoked fictive locomotion. Mechanical stimulationof the tail elicited long-lasting sequences of airstepping inthe spinal neonates and only a few steps in sham-operated rats.In vitro experiments made simultaneously on spinal and sham animalsconfirmed the increased excitability of the CPGs after spinalization.A left-right alternating locomotor pattern was observed at P1-P3.Both types of experiments showed that the pattern was disorganizedat P6-P7, and that the left-right alternation was lost. Alternationwas restored after the activation of serotonergic 5-HT₂ receptorsin vivo. These results suggest that descending pathways, in particularserotonergic projections, control the strength of reciprocal inhibitionand therefore shape the locomotor pattern in the neonatalrat.

Key words: central pattern generators; locomotion; development; descending pathways; serotonin; spinal cord transection

  Introduction

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

It is well established that the basic rhythmic activity underlying locomotion is generated by interneuronal networks withinthe spinal cord (Grillner and Wallén, 1985), defined as the centralpattern generators (CPGs). These are functional at birth in therat, as shown by experiments on in vitro spinal cord preparationsisolated from neonates (Cazalets et al., 1992). Pharmacologicalactivation of the CPGs evokes a fictive locomotor pattern consistingof alternation both between the motor bursts on the left and rightsides of the spinal cord and between flexors and extensors onone side (Kiehn and Kjaerulff, 1996). The same kind of experimentsmade on embryonic day 16 (E16; i.e., 5 d before birth) reveala motor pattern with all bursts in phase (Iizuka et al., 1998).The transition from left-right synchrony to alternation occursat E18 (Iizuka et al., 1998) and may be attributable to the maturationof reciprocal inhibitory connections between the two sides, moreprecisely to the shift of glycine-evoked potentials from excitationto inhibition (Wu et al., 1992).

These major changes in locomotor network operation occur shortly after the arrival in the lumbar enlargement of the firstaxons descending from the brainstem, suggesting that these pathwaysmay contribute to some extent to the maturation of spinal networks(Vinay et al., 2000). Projections arising from the raphe nucleiare among the earliest axons to reach the upper lumbar segmentsin the rat (Lakke, 1997). They are the source of almost all theserotonin (5-HT) in the lumbar spinal cord (for review, see Schmidtand Jordan, 2000). Serotonergic fibers start to innervate thegray matter by E17 (Bregman, 1987; Rajaofetra et al., 1989). 5-HT₂receptors play a key role in the modulation of motor functionand its recovery after spinal cord injury. First, they are foundprimarily in the ventral horn (Marlier et al., 1991; Thor et al.,1993). Secondly, their activation restores the extensor excitabilityin the spine of the cat (Barbeau and Rossignol, 1990; Miller etal., 1996) and enhances locomotor function in rats that receivedneural transplants after neonatal spinal transection (Kim et al.,1999).

In this study, we investigated the effect of suppressing inputs from supraspinal structures on the CPGs shortly after theirformation. We examined during the first postnatal week the abilityof rats to produce rhythmic motor activity with their hindlimbsafter a complete spinal cord transection at the thoracic levelon the day of birth. Animals were analyzed in two complementaryexperimental conditions: (1) Airstepping, which suppresses posturalconstraints, enabled us to examine in vivo the production of rhythmicmotor output despite the marked postural immaturity at this age(Fady et al., 1998; Brocard et al., 1999). (2) In vitro experimentsenabled us to evaluate the rhythmogenic properties of the isolatedlumbar spinal cord in the absence of sensory inflow. We reportthat, in the absence of descending modulatory inputs, the left-rightalternating locomotor pattern was lost and could be restored afterthe activation of 5-HT₂receptors.

  Materials and Methods

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

Animals. A total of 52 Wistar rats aged from postnatal day 0 (P0; defined as the first 24 hr after birth) to P7 were used.Each litter was divided into two groups: an experimental groupof approximately seven pups whose spinal cord was transected onthe day of birth and a sham group, which was operated, handled,and treated in the same way as spinal animals except for the spinalcord transection. All surgical and experimental procedures weremade to minimize animal suffering and conformed to the guidelinesfrom the French Ministry for Agriculture and Fisheries, Divisionof AnimalRights.

Surgical procedures. Rats were anesthetized by hypothermia until no reflexes could be evoked by pinching the tail or a limb.A laminectomy was made, the spinal cord was transected at theT8-T10 level with iridectomy scissors, and one or two segmentsof the cord were removed with fine forceps. The lesion cavitywas then filled with sterile absorbable local hemostat Surgicoll(Medical Biomaterial Products, Neustadt-Glewe, Germany). Skinincisions were sutured using fine thread (PDSII 6.0, Ethicon;Johnson and Johnson, Brussels, Belgium) and covered by Steri-Strips(3M Health Care, St. Paul, MN). Animals were warmed and returnedto the mother 1-2 hr after surgery. The completeness of spinalcord transection was verified postmortem by visual inspectionof the lack of continuity between the spinalstumps.

In vivo experiments. The coordination between hindlimbs was investigated during airstepping in 19 spinal animals (n = 3 atP1, n = 3 at P2, n = 2 at P3, n = 6 at P6, and n = 6 at P7). Ratswere held in a sling with the forelimbs and hindlimbs hangingon each side (see Fig. 1A) (Fady et al., 1998). Sequences of airsteppingwere triggered by pinching the tail with forceps. At least fiverecordings were obtained at 3 min intervals from each animal.Electromyographic (EMG) recordings were obtained by 100 µm silverwires (AM-Systems Inc., Carlsborg, WA) inserted into the leftand right triceps surae muscles, parallel to the muscle fibers.A reference electrode was inserted through the skin of the back.Recordings were made after a 5-10 min recovery period. Signalswere amplified, filtered (AC-coupled amplifiers; bandwidth, 70Hz to 1 kHz), digitized, and stored on a hard disk (Digidata 1200interface, pClamp 8 software; Axon Instruments, Foster City, CA;sampling frequency of 2kHz).

A group of spinal animals (n = 6) was tested at P6-P7 with the serotonergic agonist 1-[2,5-dimethoxy-4-iodophenyl]-2-aminopropane(DOI; Research Biochemicals, Natick, MA). DOI was dissolved indistilled water and injected in a volume of 1 ml/kg (0.15 mg/kg,i.p.) (Kim et al., 1999). Airstepping was tested before and afterDOIinjection.

In vitro experiments. The coordination between ventral root bursts was investigated during fictive locomotion in 33 animals:n = 2 at P2 (one spinal plus one sham), n = 6 at P3 (three spinalplus three sham), n = 10 at P4 (six spinal plus four sham), n= 8 at P5 (five spinal plus three sham), and n = 7 at P6 (fivespinal plus two sham). Animals were anesthetized by hypothermia.They were then decerebrated at a postcollicular level, eviscerated,and pinned down onto a Petri dish. Dorsal craniotomy and laminectomywere performed; the brainstem, spinal cord, and lumbar ventralroots were removed. The preparation was then pinned down in therecording chamber with the ventral side up. All dissection andrecording procedures were performed under continuous perfusionwith saline solution containing (in mM): 130 NaCl, 4 KCl, 3.75CaCl₂, 1.3 MgSO₄, 0.58 NaH₂PO₄, 25 NaHCO₃, and 10 glucose, oxygenatedwith 95% O₂ and 5% CO₂, pH adjusted to 7.4 and a temperature of24-27°C. The concentration of KCl was raised to 6 mM in sixexperiments.

Monopolar stainless-steel electrodes were placed in contact with the roots and insulated with petroleum jelly for recording.Signals were amplified, filtered, digitized, and stored in a mannersimilar to that used for EMG recordings. Fictive locomotion waselicited by bath application of N-methyl-D, L-aspartate (NMA)(8-30 µM). Serotonin (0.1-5 µM) was added in some experiments.All compounds used in these in vitro experiments were purchasedfrom Sigma (St. Louis,MO).

Statistical analysis. Subsequent analyses consisted of rectifying and integrating the recordings (time constant of 10 msecfor EMG recordings and 50 msec for root recordings). A thresholdfunction was used to determine the beginning and end of burstsof activity. The threshold was usually set to ~30% of the peakvalue. The duration of motor bursts was measured, and the middleof bursts was considered to calculate the period (defined as thetime between the midpoint of two consecutive bursts) and the phaserelationships between the left and right muscle activities (definedas the time between the cycle onset and the next burst in thecontralateral muscle, divided by the period of the ongoing cycle).The overall interlimb coordination was evaluated by means of cross-correlationanalysis (Statistica 4.5; StatSoft Inc., Tulsa, OK). The correlationcoefficient between these signals was calculated and used to evaluatethe degree of coactivation of contralateral muscles or ventralroots (Navarrete et al., 2002): the more positive this coefficient,the higher the degree of left-rightcocontraction.

All results are given as means ± SEM. The test used for each statistical analysis is indicated in Results and figure legends.The Student's test and the Mann-Whitney test were used to comparetwo groups of data that followed Gaussian and non-Gaussian distributions,respectively (Prism 2; Graphpad Software Inc., San Diego, CA).One-way ANOVA with the Tukey post-test was used for statisticalanalysis between more than two groups. Phase data were multipliedby 360° to be analyzed by circular statistics (Oriana; KovachComputing Services, Anglesey, UK). The statistical parametersused in the present study are based on the concept of the meanvector. A group of observations (or individual vectors) have amean vector that can be calculated by combining each of the individualvectors. The mean vector has two properties; its direction (themean angle) and its length (referred to using the letter r). Thelength ranges from 0 to 1; larger numbers indicate that the observationsare clustered more closely around the mean than lower numbers.The SEM and thereby the 99% confidence interval are calculatedbased on the length of the mean vector (r). Rayleigh's uniformitytest was used to determine whether the phase values were distributedin a uniform manner: a probability less than the chosen significancelevel of 0.05 indicates that the data are not distributed uniformlyand that they show evidence of a preferred direction. The Watson'sF test was used to compare two samples to determine whether theirmean angles differedsignificantly.

  Results

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

Increased excitability of the CPGs for locomotion after neonatal spinal cord transection

Mechanical stimulation of the tail in the animals with the spinal cord transected at birth elicited long-lasting sequencesof airstepping (53.8 ± 3.8 sec; n = 35) (Fig. 1A,B). Three phasescould be distinguished: (1) No clear pattern of motor activitywas detectable in the first 2-3 sec after the sensory stimulation.(2) A rhythmic motor pattern was observed in the hindlimbs duringthe next ~20 sec (Fig. 1C). (3) Hindlimb movements were more variableat the end of each sequence, as illustrated by the fluctuationsin the period (Fig. 1C, from about the 26th step onward). Theperiod increased significantly with time within a given sequenceof airstepping (589 ± 13 msec, n = 336 for the first 25 steps;684 ± 16 msec, n = 289 beyond the 25th step; p < 0.001; Mann-Whitneytest). The same stimulation applied to sham-operated neonatestriggered only the initial phase mentioned above and a few steps(data not shown) (see also Robinson and Goldberger, 1986a, fordata on neonatal cats). This is consistent with recent observationsby Lev-Tov et al. (2000) that tail stimulation in hindlimb/tail-spinalcord preparations of the neonatal rat induces six to seven burstsin lumbar ventral roots with left-right alternation. The enhancedmotor response after spinal cord section may be attributable toan increased excitability of the CPGs. In vitro experiments wereperformed to test this hypothesis.

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Figure 1. Tail stimulation triggers long sequences of airstepping in cord-transected neonates. A, Experimental device adapted from Fady et al. (1998). Animals were supported by means of an adjustable sling. The tail was pinched with a forceps. B, Rectified EMG activities from left and right ankle extensor muscles during airstepping induced by tail pinch (horizontal bar) in a 2-d-old rat that had been spinalized at birth. Bottom traces are shown at an extended time base to illustrate the pattern, consisting of left-right alternation. C, Evolution of the period and burst proportion (burst duration/period) in the left ankle extensor muscles during the episode of airstepping illustrated in B.

The application of NMA (8-20 µM) (Fig. 2A) to the in vitro isolated spinal cord evoked a stable rhythmic motor pattern inboth spinal (Fig. 2B) and sham (Fig. 2C) animals at P2-P3. Fourexperiments were performed simultaneously on both a sham and aspinal animal from the same litter. Both spinal cords were inthe same chamber and superfused equally. This enabled us to comparethe excitability of lumbar networks in the same experimental conditions.In all of the experiments, the threshold NMA concentration totrigger motor bursts in lumbar ventral roots was lower (averagedifference, 3.5 ± 1 µM; n = 4), and the latency of these burstsrelative to the perfusion onset was shorter (average difference,77 ± 21 sec; n = 9 NMA concentrations tested) in spinal animalsthan in shams (Fig. 2D) (p < 0.01; paired t test). These resultsdemonstrate that the excitability of the CPGs for locomotion isincreased after removing the influence of supraspinal structureson the lumbar cord on the day of birth.

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Figure 2. The excitability of CPGs is increased in neonates spinalized at birth. A, In vitro experiments on spinal cord preparations (T9-S4) isolated from two 2-d-old rats issued from the same litter. One animal had been spinalized at birth (spinal), and the other one had been operated in the same way except for the spinal cord transection (sham). B, C, Rectified ventral root (VR) activities from the spinal (B) and the sham (C) animals during fictive locomotion induced by NMA. Locomotor-like activity was characterized by alternation both between right and left ventral root activities and between L3 and L5 bursting on the same side. Dashed lines indicate the approximate peak of bursts occurring in the right L3 ventral root. D, Relationship between the latency of ventral root bursting (relative to the onset of NMA perfusion) and the NMA concentration in spinal ( $open circle$ ) and sham ( $black-square$ ) animals.

Evolution of the locomotor pattern after spinal cord section

We analyzed in spinal animals the pattern of airstepping between the 5th and the 24th steps to examine network operation inthe most stable phase (see above). Figure 3 shows recordings fromthe left and right ankle extensor muscles in two rats, at P3 (Fig.3A₁) and P6 (Fig. 3B₁). Activities were alternating in the formerand in phase in the latter. As a result, the cross-correlogramcomputed from these activities showed that the peak near zerowas negative at P3 (Fig. 3A₂) and positive at P6 (Fig. 3B₂). Thedistribution of the phase relationships of one EMG burst relativeto the contralateral activity observed in all the spinal animalsat P1-P3 confirmed the left-right alternating pattern, with anangle of the mean vector of 174.7 ± 5.1° (Fig. 3C₁) (n = 294 cyclesin seven animals). The direction of the mean vector switched to20.9 ± 10.1° at P6-P7 (Fig. 3C₂) (n = 289 cycles in seven animals).However, phase relationships were much more widely distributedin old than in young spinal rats, as revealed by the shorteningof the mean vector with age (r = 0.23 at P6-P7 and 0.44 at P1-P3).The difference between the two distributions was highly significant(p < 0.001; Watson's F test).

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Figure 3. The left-right alternating pattern of airstepping is lost at the end of the first postnatal week in the absence of supraspinal inputs. A₁, B₁, Rectified EMG activity from left and right ankle extensor muscles in 3-d-old (A₁) and 6-d-old (B₁) spinal rats. Traces were selected 3-13 sec after the onset of the airstepping episode. Dashed lines indicate the approximate peak of bursts occurring in the right ankle extensor muscles. A₂, B₂, Cross-correlograms between the left and right EMG recordings illustrating the out-of-phase relationship at P3 (A₁) and a synchronization at P6 (B₁) between the bursts recorded in the two extensor muscles. Cross-correlation analysis was computed from 20 sec of airstepping activity. C₁, C₂, Circular histograms showing the distribution of phase relationships between left and right motor bursts at P1-P3 (C₁) and P6-P7 (C₂). Bars indicate the number of observations within each class range (width, 10°). Data from seven animals in each age group were pooled; ~40 steps in two episodes were selected for each animal. The mean vector angle was 174.7 ± 5.1° (n = 294) at P1-P3 and 20.9 ± 10.1° (n = 289) at P6-P7; the length of the mean vector was 0.44 and 0.23, respectively. The 99% confidence interval is illustrated.

The correlation coefficient between the two EMG activities, calculated during each episode of airstepping, was significantlyhigher at the end of the first postnatal week than in P1-P3 animals(Fig. 4A) (p < 0.001; t test). This indicates that the degreeof coactivation of left and right ankle extensor muscles increasedwith age in spinal rats. The mean period was similar at all ages(Fig. 4B) (p > 0.05; Mann-Whitney test). The burst duration, normalizedto cycle duration, increased significantly during this period(Fig. 4B) (p < 0.001; t test). Both the lengthening of EMG burstsand the change in the motor pattern may contribute to the improvementin the correlation between opposite sides.

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Figure 4. The degree of coactivation of left and right ankle extensor muscles during airstepping increased with age in spinal rats. A, Mean correlation coefficient between left and right EMG activities during 10-20 sec episodes of airstepping (40 episodes in 8 animals at P1-P3 and 71 episodes in 12 rats at P6-P7). ***p < 0.001; t test. B, Period of airstepping activity and burst proportion (burst duration/period) in the two age groups. Approximately 20 steps were considered (from the 5th to the 25th step) for analysis in each airstepping episode (314 steps taken into account). ns, Not significant; p > 0.05; Mann-Whitney test. ***p < 0.001; t test.

At P4-P6, the NMA-induced motor rhythm observed in vitro in spinal animals was irregular, as shown by the recordings illustratedin Figure 5A₁ from a pair of lumbar ventral roots. Some burstsof activity in the left and right ventral roots were in phase,whereas in between them, some other bursts (usually of smalleramplitude) exhibited a left-right alternating pattern. The valueat the center of symmetry (delay = 0) of the cross-correlogramcomputed from this activity was positive, indicating that theleft and right ventral root activities are in phase overall (Fig.5A₂). Similar results were obtained in all of the spinal animalstested at P4-P6 (n = 10) (Fig. 6A,C), whatever the concentrationof NMA used (10-25 µM). The mean correlation coefficient was positivein spinal animals (Fig. 5B) (29 applications of NMA in 10 experiments)and negative in shams (10 applications on four spinal cords).The difference between the two animal groups was highly significant(p < 0.001; Mann-Whitney test). Thus, the suppression of supraspinalinfluences on lumbar segments at birth leads to a disorganizationof the left-right alternating locomotor pattern within 4-6 d.

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Figure 5. The in vitro NMA-induced locomotor-like rhythm is disorganized in spinal rats at P4-P6. A₁, Ventral root (VR) activities induced by NMA in a spinal rat at P5. A₂, Cross-correlogram between left and right L5 ventral root signals. The analysis was computed from 2 min of a locomotor-like activity similar to that illustrated in A₁. B, Mean correlation coefficient between left and right ventral root activities. Spinals, Twenty-nine applications of NMA in 10 experiments; shams, Ten applications on four spinal cords. ***p < 0.001; Mann-Whitney test.

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Figure 6. 5-HT in vitro switches the NMA-induced disorganized rhythm toward a left-right alternating pattern in spinal rats. A, B, Rectified ventral root (VR) recordings at P6 in the presence of NMA alone (A) or together with 5-HT (B). Dashed lines indicate the approximate peak of bursts occurring in the left L3 ventral root. C, Cross-correlograms between left and right L3 ventral root signals computed from 2 min of activity induced by NMA (solid line) or NMA plus 5-HT (dotted line). Arrowheads point to the successive peaks in the correlogram.

Serotonin promotes the left-right alternating pattern

We tested serotonin on P4-P6 spinal animals in vitro because it is known to improve the NMA-induced locomotor rhythm whenadded to the bath (Cazalets et al., 1992). Spinal cord transectionmarkedly reduces the 5-HT level in the lumbar enlargement withina few days (for review, see Schmidt and Jordan, 2000). Becausethe number of receptors or their binding affinity increases inthe absence of 5-HT (Gao and Ziskind-Conhaim, 1993; Kim et al.,1999), the spinal cords of spinalized rats might be more sensitiveto 5-HT than those of sham animals. Therefore, we examined theaction of 5-HT at concentrations 10-100 times lower than thoseusually used with this preparation. Even at these low concentrations(~0.1 µM), 5-HT induced a marked increase in the ventral rootactivity (compare the baselines in Fig. 6A,B). Although a tonicactivity was dominant in 7 of 10 preparations tested with 5-HTat low concentrations, a phasic fluctuation of activity was observedin the remaining three animals (Fig. 6B). In the latter experiments,left and right ventral root activities were alternating in thepresence of 5-HT, whereas an overall synchronous pattern was visiblein the presence of NMA alone (Fig. 6A). As a result, the peaknear zero in the cross-correlograms was shifted from a positiveto a negative value after 5-HT (Fig. 6C, solid and dotted lines,respectively, Fig. 7). The successive correlation peaks were decayingmoderately (~25%) in the presence of 5-HT, whereas a substantialdecline (~80%) was observed with NMA alone (Fig. 6C, arrowheads),indicating that 5-HT stabilized the period of the rhythm, in additionto shifting the overall pattern from left-right synchrony to alternation.In six experiments on P4-P6 spinal animals, NMA was applied beforeand after the concentration of extracellular potassium had beenraised from 4 to 6 mM to test whether an increased network excitabilitycould mimic the effect of 5-HT (Fig. 7). The correlation coefficientbetween left and right ventral root activities was not significantlydifferent in both conditions (0.05 ± 0.09 in 4 mM potassium and0.18 ± 0.06 in 6 mM; p > 0.05; paired t test). In three of thesix preparations tested with increased potassium concentrations,left and right ventral root activities were alternating in thepresence of 5-HT (4 mM potassium) (Fig. 7, bottom). This shiftedthe mean correlation coefficient toward negative values ( $-$ 0.09± 0.09; n = 6; p > 0.05). Thus, the improvement of left-rightalternation by 5-HT in spinal animals may not be related to anincreased excitability of locomotor networks but rather to a specificaction of 5-HT on left-right coordinating pathways.

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Figure 7. Increasing the excitability of the network does not mimic the effect of 5-HT. Cross-correlograms between left and right L3 ventral root signals computed from 2 min of activity induced by NMA before (top) and after (middle) increasing the extracellular concentration of potassium from 4 to 6 mM, or NMA plus 5-HT (bottom) are shown.

We tested the effects of DOI, an agonist acting directly at 5-HT_2A/2C receptors, on the pattern of airstepping of spinal ratsat P6-P7 (n = 6). The background activity in ankle extensor musclesincreased within the first 3-5 min after the DOI injection (datanot shown). Airstepping was tested every 3 min before (5-10 trials)and after (10-15 trials) DOI injection. Cross-correlation analysiswas performed for each sequence on the first 10 sec of stablerhythm. Figure 8A₁-A₄ shows the results from a single experiment.No clear peak was visible near zero in the control cross-correlation,and the value at zero was positive (Fig. 8A₁); a downward peakappeared 5 min after DOI injection (Fig. 8A₂) and shifted to negativevalues 3 min later (Fig. 8A₃). The whole cross-correlogram wascentered on the x-axis 20 min after injection (Fig. 8A₄). Theemergence of a left-right alternating pattern is indicated bya negative peak appearing at the center of the cross-correlationwith DOI. This is confirmed by comparing, in the same experiment,the distributions of phase relationships between contralateralEMG activities before (Fig. 8B₁) and after (Fig. 8B₂) the injectionof the 5-HT₂ agonist.

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Figure 8. The left-right alternating pattern reappears in vivo after the activation of 5-HT₂ receptors. A₁-A₄, Cross-correlograms between left and right ankle extensor EMG signals during airstepping, before (A₁) and at different times (A₃, A₄) after the injection of DOI. The analysis was run on 10 sec of airstepping activity, starting 1 sec after the episode onset. B_{1, 2}, Distribution of phase relationships between left and right motor bursts before (B₁) and after (B₂) the injection of DOI. Same experiment as in A. Mean vector angle: 98.4 ± 9.5°, n = 107 (length, 0.4) before DOI; 181.7 ± 4.1°, n = 153 (length, 0.68) after DOI. The 99% confidence interval is represented. C, Mean correlation coefficient at P1-P3, P6-P7 (identical to Fig. 4A), and P6-P7 after DOI injection (48 episodes analyzed in 6 animals). *p < 0.05; **p < 0.01; ***p < 0.001; one-way ANOVA with Tukey post-test.

Phase relationships were analyzed in four animals; they were always modified significantly by DOI (p < 0.001; Watson's F test).Before DOI injection, the angle of the mean vector was 89 ± 12.4°(n = 292 steps in four animals pooled); however, note that themean vector was short (r = 0.19), indicating a relatively uniformdistribution. After DOI, the mean vector direction switched to177 ± 4° (n = 442 steps) and the phase relationships were clusteredmore closely around the mean angle than before DOI, as indicatedby the increased length of the mean vector (r = 0.42). The periodincreased significantly after DOI in two animals (~20%; p < 0.001;Mann-Whitney test), whereas no effect was observed in the remainingtwo animals (p > 0.05; Mann-Whitneytest).

The correlation coefficient between the two EMG activities was significantly reduced after DOI injection compared with before(Fig. 8C) (one-way ANOVA with Tukey post-test; 48 episodes examinedafter DOI in six animals; 71 episodes without DOI in 12 animals).The correlation coefficient after DOI injection was still largerthan at P1-P3 (40 episodes in eight animals). These data showthat DOI reduces the degree of cocontraction of the left and rightankle extensor muscles, which is consistent with the emergenceof an alternatingpattern.

  Discussion

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

Our results demonstrate that the removal of the supraspinal influences on lumbar sensorimotor networks at birth increasestheir excitability. The left-right alternating locomotor patternobserved in young spinalized animals was gradually lost duringthe first postnatal week and reappeared after activating 5-HTreceptors. These data provide new perspectives on the role ofdescending pathways in patterngeneration.

Spinal cord transection releases locomotion in neonates

Stimulation of the tail triggered long-lasting sequences of airstepping in spinalized neonates (Fig. 1) and only a few stepsin sham animals (Lev-Tov et al., 2000). Previous studies on kittensshowed that some motor behaviors are suppressed by descendingsystems in newborns and are therefore released after spinal transectionat birth (Robinson and Goldberger, 1986a). At least two mechanismsmay account for this difference after spinal transection: (1)Monoamines depress several sensory pathways (for review, see Jankowska,2001). Therefore, removal of this control by spinal transectionmay increase the motor effects of tail stimulation. (2) In addition,in vitro experiments indicated that the excitability of lumbarnetworks was increased in spinalized animals (Fig. 2). Spinalcord transection results in the removal of a number of inhibitorydescending pathways (Holstege, 1991; for review, see Newman, 1995),thus leading to the disinhibition of spinal networks. The developmentof segmental inhibition may also be reduced in the absence ofdescending systems (Robinson and Goldberger, 1986b).

The presence of higher centers may be critical for the expression of a left-right alternating pattern in neonates

The overall pattern of airstepping switched in cord-transected animals from left-right alternation at P1-P3 to synchrony atP6-P7 (Figs. 3-5). This is consistent with a previous study, whichshowed synchronous airstepping during the first two postnatalweeks in kittens spinalized at birth (Bradley and Smith, 1988).Interestingly, these authors observed more alternation duringtreadmill stepping than during airstepping (~40 vs ~3% of alternatingsteps, respectively), suggesting that rhythmic ground contactmay promote an alternating gait. Thus, airstepping may accuratelyrepresent "the natural capacity of the pattern-generating circuitsto regulate stepping" (Bradley and Smith, 1988). The age-relatedswitch observed in the present study in spinal animals towarda more synchronous gait could at initially imply a change in pacefrom walk to gallop. However, three arguments suggest that thisis unlikely to be the case: (1) The period was similar in bothage groups. (2) The burst duration relative to period in ankleextensor muscles was increased in older rats, instead of decreasedas expected from gallop. (3) The pattern was rather well phase-lockedon alternation in younger rats, as indicated by the low variability,whereas it was more variable in older rats. The increased variabilityat P6-P7 suggests that the overall synchrony is obtained by defaultand results more from the disorganization of the alternating patternthan from the emergence of a newpattern.

The alternation of muscle activities between the two hindlimbs relies on mutual inhibition of the networks on the two sidesof the cord (Grillner et al., 1991). This inhibition involvesboth crossed reciprocal inhibitory interneurons and a disynapticpathway with crossed excitatory interneurons (Kjaerulff and Kiehn,1997). A left-right alternating pattern reappeared at P6-P7, whenone of the modulatory inputs from the brainstem was restored artificially(Figs. 6-8) (5-HT in vitro and DOI in vivo). This reversibilitysuggests that no structural change in the network underlies thedisorganization of the pattern after spinalization; instead, descendingpathways may control the strength of reciprocal inhibition (McDearmidet al., 1997). Higher centers use a vast array of signaling moleculesto modulate spinal locomotor networks. Depending on the targetneuron within the network on which these neuromodulators act,they may enable the emergence of distinct motor patterns, in amanner similar to what has been demonstrated in the stomatogastricganglion (Combes et al., 1999; Nusbaum et al., 2001; Swensen andMarder, 2001; Thirumalai and Marder, 2002). The developmentalacquisition of the alternating pattern occurs before birth (Ozakiet al., 1996), at a time when the first monoaminergic projectionsreach the lumbar enlargement (Rajaofetra et al., 1989). It isassumed that this switch from left-right synchrony to alternationis attributable to a change of glycine-evoked potentials fromexcitation to inhibition (Nishimaru and Kudo, 2000). In additionto this contribution, the present study suggests that the onsetof modulation of left-right coordinating pathways by descendingpathways may be an important step in the maturation of the locomotorpattern. Removing this modulation during a critical period afternetwork formation may lead to a dedifferentiation or a disorganizationof the pattern. The degree of disorganization may depend on theage at which the spinal cord is transected: hindlimb movementsduring airstepping are predominantly alternating in kittens spinalizedat P14 and synchronous in kittens spinalized at birth (Bradleyand Smith, 1988). However, the percentage of synchronous stepsremains high, even 2 months after a spinalization at P14 (~40%;seebelow).

5-HT may regulate the left-right coordinating pathways

5-HT has been proposed to be critical for the selection between alternate reflex pathways in the cat (Aggelopoulos et al.,1996), enabling the crossed inhibition of contralateral motoneuronsby group II muscle afferents, to the detriment of a crossed excitation,which is observed in the spinal animal. The present study suggeststhat 5-HT may strengthen the reciprocal inhibition via 5-HT_2A/2Creceptors (Fig. 8). Activation of these receptors enhances glycineand/or GABA responses in various spinal neurons in the rat (Xuet al., 1996, 1998; Li et al., 2000) and spontaneous IPSCs inpyramidal neurons (Zhou and Hablitz, 1999). Serotonin may actat a presynaptic level by causing a presynaptic facilitation ofglycine release (Mintz and Korn, 1991) in the teleost Mauthnercell, or even by increasing the number of transmitter vesiclesavailable for release (Wang and Zucker, 1998). It should be notedthat 5-HT reduces the reciprocal inhibition in Xenopus laevis(McDearmid et al., 1997); these effects are likely mediated viapresynaptic 5-HT_1A receptors (Wedderburn and Sillar, 1994). Whetherthese receptors mediate inhibitory effects on reciprocal inhibitionin the neonatal rat remains to be tested. The net effect of 5-HTin vitro is excitatory and may mask an inhibition (Liu et al.,2000).

Serotonin-releasing neurons within the spinal cord are an integral part of the locomotor system in the adult lamprey (Zhangand Grillner, 2000). The spinal 5-HT level may also be criticalfor the proper operation of networks in the neonatal rat. A depletionof 5-HT by daily injections of P-chlorophenylalanine from theday of birth in the rat leads, within a few days, to impairedinterlimb coordination during locomotion (Myoga et al., 1995)and posture (Pflieger et al., 2002). The NMDA-induced locomotoractivity observed in the neonatal rat spinal cord in vitro isabolished by 5-HT receptor antagonists, suggesting that an interplaybetween 5-HT and NMDA receptor actions is important for the productionof rhythmic locomotor-like activity in this preparation (Macleanet al., 1998; Maclean and Schmidt, 2001). The 5-HT level is unchangedbelow the spinal cord transection in adult rabbits during thefirst few days after the operation; 5-HT then disappears suddenlyto almost insignificant values (Andén et al., 1964). A similartime course for the disappearance of 5-HT in the rat spinal cordafter neonatal transection would account for both observationsmade in the present study that the airstepping pattern is alternatingat P1-P3 (Figs. 1, 3) and that the activity recorded in vitroat the same age after spinal cord transection was quite similarto that obtained in shams, except for the threshold NMA concentration(Fig. 2). In addition, 5-HT may facilitate the left-right coordinatingpathways on a long-termbasis.

Do descending modulatory inputs shape the locomotor pattern in adult mammals?

The descending modulatory input to spinal locomotor networks may be important not only during ontogeny, as suggested by thepresent study, but also in the adult. Although it is quite clearthat the basic circuitry is restricted to the spinal cord, theimportance of descending pathways in modulating synaptic interactionswithin the network, thereby shaping the locomotor pattern, hasbeen mostly neglected. This is partially attributable to the factthat, after spinalization in adult cats, a hindlimb locomotorpattern close to normal can be obtained by training (Barbeau andRossignol, 1987; De Leon et al., 1998; Edgerton et al., 2001)or pharmacological stimulation (Jankowska et al., 1967a,b; Grillnerand Zangger, 1979) [for fictive locomotion, see Forssberg andGrillner (1973); for treadmill locomotion, see Rossignol (1996)].However, most experiments used monoamines, and the contributionof these substances to shaping the pattern (i.e., not only totrigger activity in the spinal networks) may have been underestimated.Training may induce an activity-dependent tuning of the inhibitorysynaptic strengths in the network (Soto-Trevino et al., 2001;Traub, 2001) that may compensate for the absence ofmonoamines.

  FOOTNOTES

Received July 30, 2002; revised Dec. 2, 2002; accepted Dec. 11, 2002.

^* J.-C.N. and J.-F.P contributed equally to thiswork.

This work was supported by the Association libre pour la Recherche sur la Moelle Epinière and the Fondation pour la RechercheMédicale (France) (J.-C.N.), and by the Fonds pour la Rechercheen Santé du Québec and the Natural Sciences and EngineeringResearch Council of Canada (J.-F.P.).

Correspondence should be addressed to Dr. Laurent Vinay, Institut de Neurosciences Physiologiques et Cognitives, Centre Nationalde la Recherche Scientifique, 31 chemin Joseph Aiguier, F-13402Marseille, Cedex 20, France. E-mail: vinay{at}dpm.cnrs-mrs.fr.

  References

TOP
ABSTRACT
Introduction
Materials and Methods
Results
Discussion
REFERENCES

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