Loss of Synaptic Depression in Mammalian Anterior Cingulate Cortex after Amputation

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The Journal of Neuroscience, November 1, 1999, 19(21):9346-9354

Loss of Synaptic Depression in Mammalian Anterior Cingulate Cortex after Amputation
Feng Wei, Ping Li, and Min Zhuo
Departments of Anesthesiology, and Anatomy and Neurobiology, Washington University Medical Center, Washington University School of Medicine, St. Louis, Missouri 63110

  ABSTRACT

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Two forms of activity-dependent long-term depression (LTD) in the CNS, as defined by their sensitivity to the blockade ofNMDA receptors, are thought to be important in learning, memory,and development. Here, we report that NMDA receptor-independentLTD is the major form of long-term plasticity in the anteriorcingulate cortex (ACC). Both L-type voltage-gated calcium channelsand metabotropic glutamate receptors are required for inducingLTD. Amputation of a third hindpaw digit in an adult rat inducedrapid expression of immediate early genes in the ACC bilaterallyand caused a loss of LTD that persisted for at least 2 weeks.Our results suggest that synaptic LTD in the ACC may contributeto enhanced neuronal responses to subsequent somatosensory stimuliafteramputation.

Key words: synaptic plasticity; long-term depression; immediate-early gene; cingulate cortex; amputation; glutamate

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The adult human somatosensory cortex is often represented with a distorted human figure on its surface to illustrate the somatotopicmap. For a long period of time, it had been thought that thisfigure remained relatively stable in adults. Studies over thepast 20 years have dramatically changed this view (Wall, 1988;Kaas, 1991; Gilbert and Wiesel, 1992; Merzenich and Sameshima,1993; Ramachandran, 1993; Weinberger, 1995; Gilbert, 1996; Buonomanoand Merzenich, 1998; Kilgard and Merzenich, 1998). Cortical representationsin the mammalian brain are rather dynamic and can be modifiedby experience. Not only do plastic changes occur in adults, butthey can happen on a rapid time scale (from a few minutes to severalhours). It has been proposed that use-dependent changes in synapticstrength, such as long-term potentiation (LTP) and long-term depression(LTD), may serve as key synaptic mechanisms of cortical plasticity(Tsumoto, 1992; Bliss and Collingridge, 1993; Bear and Malenka,1994; Linden, 1994; Lisman, 1994; Larkman and Jack, 1995; Nicolland Malenka, 1995; Singer, 1995; Bear and Abraham, 1996).

Although cortical reorganization acts as an adaptive mechanism during development and learning, it could also play a detrimentalrole in traumatic events, such as the loss of a limb. It has beendemonstrated that cortical reorganization occurs after limb ordigit amputation (Wall, 1977; Merzenich et al., 1984; Pons etal., 1991; Ramachandran et al., 1992, 1995; Florence et al., 1998;Jones and Pons, 1998; Kaas, 1998; Merzenich, 1998). Most humanamputees experience phantom limb sensation or phantom pain (Shermanet al., 1980; Melzack, 1990; Jensen and Rasmussen, 1994), andthe amount of cortical reorganization correlates with the extentof phantom pain (Flor et al., 1995; Birbaumer et al., 1997; Lorenzet al., 1998). A critical question is whether synaptic mechanisms,which are implicated in the learning process, may contribute toplastic changes in the CNS afteramputation.

The anterior cingulate cortex (ACC) forms a large region around the rostrum of the corpus callosum and is involved in emotionaland attentive responses to internal and external stimulation (Devinskyet al., 1995; Rainville et al., 1997; Tolle et al., 1999). Recently,neuroimaging and electrophysiological studies in humans have shownthat pain activates several limbic sites, including the ACC (Talbotet al., 1991; Vogt et al., 1996; Davis et al., 1997; Derbyshireet al., 1998; Lenz et al., 1998; Paulson et al., 1998; Hutchisonet al., 1999). Further experiments demonstrate that the ACC receivesnociceptive inputs in animals (Kenshalo et al., 1988; Sikes andVogt, 1992; Traub et al., 1996; Vogt et al., 1996; Koyama et al.,1998). A previous report showed that only short-term potentiationbut not LTP was recorded in vitro in slices from the ACC (Sahand Nicoll, 1991). LTD has not been investigated. In the presentstudy, we first examined whether LTD serves as a form of synapticplasticity in slices of adult ACC. We then examined the possibleeffect of hindpaw digit amputation on the synaptic plasticityin theACC.

  MATERIALS AND METHODS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

In vitro electrophysiology. The ACC slices (200 µm) from 7- to 21-d-old Sprague Dawley rats (Harlan Sprague Dawley, Indianapolis,IN) were used for whole-cell patch-clamp recordings. Under visualguidance recordings in individual layer II/III, cortical pyramidalcells were made using 3-5 M $Omega$ electrodes without fire polishing.Recording electrodes contained (in mM): 110 Cs-MeSO_3, 5 MgCl₂,1 EGTA, 40 HEPES sodium, 2 MgATP, and 0.1 Na₃GTP, pH 7.2. Theosmolarity was adjusted to 295-300 mOsm. Membrane potential wasclamped at $-$ 70 mV (liquid junction potential not corrected). Seriesresistance was 15-40 M $Omega$ and monitored throughout the experiments.Synaptic EPSCs were evoked by a bipolar stimulating electrodeplaced at layer V. Picrotoxin (100 µM) was added to the perfusionsolution. Currents were filtered at 1 kHz and digitized at 5kHz.

For field potential recordings, adult male Sprague Dawley rats (8-10 weeks) were anesthetized with 2% halothane and decapitated.Coronal ACC slices, 400-µm-thick, were rapidly prepared and maintainedin an interface chamber at 28°C in which they were perfused withoxygenated (95% O₂ and 5% CO₂) artificial CSF (ACSF) consistingof (in mM): 124 NaCl, 4.4 KCl, 25 NaHCO₃, 1.0 NaH₂PO₃, 2.0 CaCl₂,2.0 MgSO₄, and 10 D-glucose. A bipolar tungsten stimulating electrodewas placed in layer V, and extracellular field potentials wererecorded with a glass microelectrode (filled with ACSF) insertedinto layer II/III. Responses were evoked at 0.02 Hz. In some experiments,two-pathway experiments were performed. A surgical cut was madebetween two stimulating electrodes. Responses to paired-pulsestimulation (with a 50 msec interval) were used to confirm theindependence of the two pathways. Low-frequency stimulation wasonly delivered to one pathway. In other experiments, we also recordedsynaptic responses from the parietal cortex (PC) (see Fig. 7).Drugs were freshly prepared: voltage-gated L-type calcium channelblocker nimodipine (10 µM), NMDA receptor antagonist AP-5 (100µM), and metabotropic glutamate receptor (mGluR) antagonist (+)- $alpha$ -methyl-4-carboxylphenylglycine(MCPG) (500 µM). Slices were pretreated with a drug for at least30 min before low-frequencystimulation.

Immunocytochemistry. Under brief anesthesia with halothane, the third digit of the unilateral hindpaw of adult male rats wasamputated. At 15 min (n = 3 rats), 45 min (n = 6), 90 min (n =4), 120 min (n = 4), 2 d (n = 4), and 2 weeks (n = 4) after theamputation, rats were deeply anesthetized with halothane and perfusedtranscardially with 100 ml of saline, followed by 500 ml of cold0.1 M phosphate buffer (PB) containing 4% paraformaldehyde. Shamoperations without amputation were performed as controls (n =10). The brains were removed, post-fixed for 4 hr, and then cryoprotectedby storing in 30% sucrose in 0.1 M PB for 2 d at 4°C. Coronalsections (25-µm-thick) through the ACC were cut using a cryostat.Sections from sham and experimental animals were processed simultaneouslyfor immunostaining of three immediate-early gene (IEG)-encodedproteins. Primary rabbit antibodies used included: anti-c-Fos(1:20,000; Oncogene Science, Uniondale, NY), anti-phosphorylatedcAMP response element-binding protein (pCREB) (1:1000; UpstateBiotechnology, Lake Placid, NY), and anti-NGFI-A (1:5000; a giftfrom Dr. Jeffrey D. Milbrandt at Washington University, St. Louis,MO). Secondary reactions with biotinylated goat anti-rabbit immunoglobulin(1:400; Vector Laboratories, Burlingame, CA) for 1 hr were followedby avidin-biotin-peroxidase complexes (1:100; Vector Laboratories)for 1 hr. Diaminobenzadine with nickel was used as the final chromogen.In addition, for identification of AMPA receptor distributionin the cortical area, some ACC sections from normal rats (n =3) were performed with anti-GluR2/3 antibody(1:200; Chemicon,Temecula, CA) and then processed as above. Alternate sections,incubated in the absence of a primary antibody as an immunocytochemicalcontrol, showed no immunostaining. Sections from the bilateralACC from 1.0 mm rostral to 0.8 mm caudal to bregma (Paxinos andWatson, 1997) were used for quantity. The number of IEG-expressedcells within an area of 750 × 600 µm, including layers II-VI ofthe ACC, was plotted and counted. Two-way ANOVA was used to comparethe number of labeled cells in different groups of animals. Posthoc Scheffe F test was used to identify significant differences.p < 0.05 was considered statisticallysignificant.

  RESULTS

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Glutamate-mediated postsynaptic transmission in the ACC

Previous studies indicated that glutamate is the major fast excitatory neurotransmitter in the ACC (Sah and Nicoll, 1991;Tanaka and North, 1994). Thus, we first examined distributionof immunoreactivity for glutamate receptor subunit 2/3, a representativeof AMPA receptors. Many neurons in layers II-V of the ACC areawere labeled. Most ACC pyramidal neurons in layers II/III andV display intense GluR2/3 immunostaining in the perikarayal cytoplasmand proximal dendrites (Fig. 1A). Whole-cell patch-clamp recordingsfrom ACC pyramidal cells showed that fast EPSCs were elicitedby delivering focal electrical stimulation to layer V (Fig. 1B).When cells were held at $-$ 70 mV, EPSCs were completely blockedby the AMPA/kainate receptor antagonist CNQX (10 µM) (Fig. 1C).Consistent with a previous report (Tanaka and North, 1994), EPSCswere subject to opioid modulation. [D-Pen^2,5]-enkephalin (DPDPE) (1 µM), a selective $delta$ receptor agonist, significantlyinhibited EPSCs (n = 5; 57.3 ± 11.3% of control; p < 0.05) (Fig.1D).

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Figure 1. Excitatory synaptic transmission in the ACC. A, Laminar distribution of GluR2/3-immunoreactive neurons in the ACC (left) and high magnification of the labeled pyramidal neurons and their proximal dendrites in layer II/III from the left photograph (right). Scale bars: left, 250 µm; right, 50 µm. B, Diagram of a cingulate cortical slice showing the placement of whole-cell patch recording, field EPSP recording, and stimulating electrodes. C, D, Whole-cell patch recording of EPSCs recorded at $-$ 70 mV holding potential in normal medium (control) or 10 min after addition of 10 µM CNQX (C) or 1 µM DPDPE (D). In a total of five experiments, CNQX blocked EPSCs, and DPDPE inhibited EPSCs to 57.3 ± 11.3% of control.

LTD induced by low-frequency stimulation

Excitatory synaptic transmission in slices from the ACC undergoes LTD. Field EPSPs recordings from ACC slices of adult ratsshowed that fast EPSPs induced by a bipolar electrode placed inlayer V were mediated by AMPA/kainate receptors, because 10 µMCNQX blocked the response (n = 5). A stimulation protocol forinducing LTD in both the hippocampus and visual cortex (1 Hz for15 min) (Dudek and Bear, 1992; Mulkey and Malenka, 1992; Kirkwoodet al., 1993) was used. Low-frequency stimulation produced long-lastingdepression of synaptic responses (Fig. 2A,B). Depression was frequencyrelated. Repetitive stimulation at 5 Hz but not 10 Hz with thesame number of pulses (n = 900) produced depression of synapticresponses (Fig. 2C,D).

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Figure 2. Low-frequency stimulation produced LTD in the ACC. A, An example that low-frequency stimulation (0.02 Hz) produced a long-lasting depression of synaptic responses. Inset, Representative records of the EPSP recorded before and 30 min after 1 Hz stimulation. B, Summary results for LTD (n = 10; 36.3 ± 6.3% of control 30 min after the stimulation; p < 0.01 compared with EPSPs before stimulation). C, D, Repetitive stimulation at 5 Hz for 3 min also produced synaptic depression (squares; n = 5; 50.4 ± 6.0% of control; p < 0.01), but 10 Hz stimulation for 1.5 min did not produce any depression (squares; n = 5; 80.8 ± 11.9% of control).

To test whether LTD in the ACC is input specific, we performed two-pathway experiments in some slices (Fig. 3). Conditioningstimulation (1 Hz for 15 min) was only delivered to one pathway.As showed in Figure 3B-D, whereas synaptic responses were significantlydepressed in the stimulated pathway (n = 6; 52.0 ± 7.3%; p < 0.01compared with EPSPs before the stimulation), synaptic responsesin the second, independent pathway were not significantly affected(101.1 ± 6.2% of control). This result indicates that LTD in theACC is input-specific.

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Figure 3. Two-pathway experiments showed that LTD is input-specific. A, Diagram of an ACC slice showing the placement of stimulating electrodes in two divided pathways (S1, S2). B, Representative records of the EPSP recorded before and 30 min after 1 Hz stimulation in the stimulated pathway (S1) and control pathway (S2). C, D, Responses to paired-pulse stimulation (with a 50 msec interval) were used to confirm the pathway-dependent induction of LTD (n = 6). Stimulation of S1 led to LTD only in the S1 pathway as shown by the synaptic response (C). D, Summary results of two-pathway experiments (n = 6).

Several types of postsynaptic receptors or channels have been reported to contribute to the induction of LTD, including voltage-gatedcalcium channels, NMDA receptors, and mGluRs (Bashir et al., 1993;Kato 1993; Boshakov and Siegelbaum, 1994; Cummings et al., 1996;Deisseroth et al., 1996; Oliet et al., 1997). To test their rolesin cingulate LTD, we performed experiments in the presence ofselective antagonists. Nimodipine (10 µM) completely blocked theinduction of LTD (Fig. 4A), although basal synaptic responseswere not significantly affected. In contrast, 100 µM AP-5 didnot affect LTD (Fig. 4B). MCPG (500 µM), a metabotropic glutamatergicreceptor antagonist, also blocked LTD (Fig. 4C). These resultssuggest that both L-type calcium channels and mGluRs are criticalfor the induction of LTD in the ACC. LTD was not affected in thepresence of picrotoxin (100 µM), a GABA_A receptor antagonist,indicating that inhibitory influences are not required for LTD(Fig. 4D).

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Figure 4. Blockade of LTD by nimodipine or MCPG. A, B, LTD was abolished in the presence of voltage-gated L-type calcium channel blocker nimodipine (10 µM; A, squares; n = 5; 96.3 ± 13.5% of control) but not NMDA receptor antagonist AP-5 (100 µM; B, squares; n = 5, 34.9 ± 15.7% of control). Slices were pretreated with a drug for at least 30 min before low-frequency stimulation. C, LTD was also blocked in the presence of an mGluR antagonist MCPG (500 µM; n = 4; 94.1 ± 20.3%; p < 0.01). D, Summary results for treatment with nimodipine, AP-5, MCPG, or GABA_A receptor antagonist picrotoxin (100 µM; n = 3; 46.1 ± 20.4%). *p < 0.01 compared with the control group.

Expression of immediate early genes after amputation

Previous studies in the somatosensory cortex showed that a large-scale functional reorganization occurs after peripheral amputationin both adult animals and humans (Wall, 1977; Merzenich et al.,1984; Pons et al., 1991; Ramachandran et al., 1992, 1995; Florenceet al., 1998; Jones and Pons, 1998; Kaas, 1998; Merzenich, 1998).However, potential plastic changes within the ACC have not beenstudied. In contrast to somatosensory cortex neurons, which havetopographical representation of the sensory receptive field ofthe body, ACC neurons often have a diffuse receptive field andrespond to stimuli applied to anywhere on the body surface (Vogtet al., 1979; Kenshalo et al., 1988; Devinsky et al., 1995; Sikesand Vogt, 1992). As a marker for synaptic activity in the ACC,the expression of two major IEGs, c-fos and NGFI-A, were examinedat different time points after the amputation. c-fos and NGFI-Aare transcription factors that are members of the leucine zipperand zinc finger families, respectively (Morgan and Curran, 1991;Munglani and Hunt, 1995). In animals receiving sham treatment,there was little expression of c-Fos and a basal level of NGFI-A(Fig. 5A, Table 1). However, we found that single-digit amputationin rats induced significant bilateral increases in the numbersof ACC cells expressing c-Fos or NGFI-A from 15 min to 2 d, withmaximum expression at 45 min (Fig. 5A, Table 1). c-fos has Ca²⁺/CRE-like sequences in its promoter regions, and its transcriptionis regulated by pCREB (Ginty et al., 1993). Significant increasesin the expression of pCREB were also found bilaterally in ACCafter amputation compared with a basal level in sham-operatedrats (Fig. 5B, Table 1). Unlike c-Fos and NGFI-A, the level ofpCREB 2 weeks later was lower than that in normal rats.

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Figure 5. Potentiation of IEG expression in the ACC after the amputation. Photomicrographs showing expression of c-Fos and NGFI-A (A) and phosphorylation of CREB (B) in the coronal ACC sections from sham animals (Ctrl) and animals at different times after the amputation of the unilateral hindpaw third digit. Scale bars, 500 µm. The numbers of c-Fos-, NGFI-A-, and pCREB-immunoreactive cells increased bilaterally after the amputation (see Table 1 for summary).


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Table 1. Expression of c-Fos, pCREB, and NGFI-A in the rat ACC after unilateral amputation of a single digit of the hindpaw

Loss of LTD after amputation

LTD is modified during development, learning, and stress in the neocortex and hippocampus (Abraham and Bear, 1996; Henschand Stryker, 1996; Kirkwood et al., 1996; Xu et al., 1997; Feldmanet al., 1998; Rittenhouse et al., 1999). We next tested whetherLTD in the ACC may be affected in rats receiving a third-digitamputation. In vitro experiments were performed in slices obtainedfrom adult rats 45 min after amputation, a time when significantincreases in the expression of the three IEGs were found (Table1). LTD was almost completely abolished in slices taken at 45min after amputation (Fig. 6B). The changes were bilateral; slicesobtained from the cingulate cortex ipsilateral or contralateralto the amputated hindpaw digit showed a similar loss of LTD (ipsilateral,n = 3; contralateral, n = 5). Similar results were obtained withstimulation at another frequency (5 Hz for 3 min) (n = 5; datanot shown). The loss of LTD persisted for many days after amputation.In slices taken 2 d (n = 5; 115.1 ± 10.7% of control 30 min afterthe stimulation) or 2 weeks (Fig. 6C) after amputation, LTD inthe ACC was abolished.

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Figure 6. Long-lasting loss of LTD in the ACC after the amputation. LTD recorded from ACC slices in sham animals (A) (n = 5; 28.4 ± 14.0%) and rats at 45 min (B) (n = 7; 76.5 ± 7.8%; p < 0.05 compared with the control group) and 2 weeks (C) (n = 5; 91.1 ± 18.3%; p < 0.05 compared with the control group) after the amputation. Inset in C, Representative records of the EPSP recorded before and 30 min after 1 Hz stimulation.

To test whether the loss of LTD after amputation may be restricted to the ACC, we performed the same experiment in the PCfrom normal and amputated animals. Low-frequency stimulation (1Hz, 15 min) produced long-lasting depression of synaptic responsesin slices from both groups of rats (Fig. 7).

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Figure 7. Selective loss of LTD in the ACC but not the PC after the amputation. A, Diagram of a cortical slice showing the placement of recording and stimulating electrodes in the PC. B, Repetitive stimulation (1 Hz, 15 min; open bar) induced a long-lasting depression of synaptic response in sham animals (open squares; n = 3; 27.6 ± 6.3% of control; p < 0.01). At 45 min after amputation of the third hindpaw digit, similar LTD was induced in slices of PC (filled squares; n = 4; 24.0 ± 11.0%). C, The amputation produced a selective loss of LTD in the ACC but not the PC areas in the same cortical slices.

  DISCUSSION

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Peripheral deafferentation or amputation could cause massive plastic changes within cortical and subcortical structures (Kaaset al., 1999). For early changes, it is likely that plastic changesmay occur between existent neuronal synapses, and for late changes,structural changes within the CNS, including formation of newsynapses, could occur. In the present study, we found that amputationof a single digit of one hindpaw caused rapid and prolonged plasticchanges in sensory synaptic responses. Altered synaptic plasticityin the ACC, a region critical for processing pain infor-mationin the CNS, may serve as an important synaptic mechanism for enhancednociceptive transmission after deafferentation oramputation.

LTD caused by repetitive stimulation in adult cingulate cortex

Two forms of LTD have been reported in the CNS, distinguished by their sensitivity to the blockade of NMDA receptor antagonists:NMDA receptor-dependent LTD and NMDA receptor-independent LTD(see Boshakov and Siegelbaum, 1994; Deisseroth et al., 1996; Olietet al., 1997). Physiological roles of NMDA receptor-dependentLTD have been indicated in several areas, such as in the visualcortex and hippocampus (Bear and Malenka, 1994). In this study,we have found that NMDA receptor-independent LTD is the majorform of synaptic depression in slices from the ACC of adult rats.Unlike the posterior cingulate cortex, LTD in the ACC did notrequire activation of NMDA receptors (Hedberg and Stanton, 1996).In contrast, activation of L-type calcium channels and mGluRsis required for the induction ofLTD.

More importantly, we demonstrate that slices of adult rats, after a third hindpaw digit amputation, fail to undergo synapticdepression induced by repetitive, low-frequency stimulation. Severalmechanisms may contribute to the loss of LTD after amputation.First, occlusion of synaptic transmission could be induced bycortical depression after amputation. However, this seems unlikelyto be the case. Basal synaptic responses to presynaptic transmissiondo not seem to be significantly different from that of controlanimals. More importantly, we found that synaptic responses toperipheral electrical stimulation were enhanced after amputation(our unpublished observations), although the exact central locifor these changes have not been determined. Second, amputationcould cause plastic changes in the postsynaptic cells and thusaffect the induction of LTD. We have shown that amputation leadsto a large-scale activation of neurons in the ACC and potentiationof synaptic transmission. Therefore, it is likely that enhancedpostsynaptic excitability contributes to the failure to induceLTD after amputation. Previous studies in both hippocampus andvisual cortex showed that postsynaptic membrane depolarizationcould determine whether synaptic transmission undergoes potentiationor depression (Stanton and Sejnowski, 1989; Artola et al., 1990;Stevens, 1990). Our results using different kinds of IEG stainingalso found that many cells in the ACC showed plastic changes ofsynaptic activity after amputation. We favor the second possibilitythat postsynaptic changes affect the induction of LTD. However,we cannot exclude possible unknown presynaptic mechanisms, whichcould also contribute to the loss of LTD byamputation.

Plasticity in the ACC after amputation

In primitive sensory neurons of invertebrates, both condition-related learning and injury of peripheral axons are reportedto cause an increase in excitability (Walters et al., 1991; Woolfand Waters, 1991). In mammalians, similar changes have been studiedin the dorsal horn of the spinal cord (Woolf, 1992). Prolongedactivation of nociceptive afferent fibers or tissue and nerveinjury induced a long-term increase in sensory transmission indorsal horn neurons, including ascending projection neurons. Theinvolvement of supraspinal structures has been less investigated,although there is cumulative evidence suggesting that many supraspinalstructures, including those that send descending projection pathways,play an important role after tissue or nerve injury (e.g., amputation).The present study shows that synaptic plasticity of excitatoryglutamatergic transmission in the ACC was altered after amputationof a single digit of the hindpaw. This, together with numerousreports using divergent approaches (Katz and Melzack, 1990; Merzenichand Sameshima, 1993), suggests that memory mechanisms in bothinvertebrates and vertebrates may have evolved from animals' adaptiveresponses to injury. Changes in glutamatergic synaptic responseshave been implicated in development, learning, and memory storage(Tsumoto, 1992; Bliss and Collingridge, 1993; Bear and Malenka,1994; Linden, 1994; Lisman, 1994; Larkman and Jack, 1995; Nicolland Malenka, 1995; Singer, 1995; Bear and Abraham, 1996). Ourresults support previous evidence of cortical reorganization inthe somatosensory cortex during learning or after amputation (Wall,1977; Merzenich et al., 1984; Pons et al., 1991; Ramachandranet al., 1992, 1995; Florence et al., 1998; Jones and Pons, 1998;Kaas, 1998; Merzenich, 1998).

Functional implications

Studies from animals and humans consistently suggest that the ACC plays an important role in nociception and pain, in additionto its important roles in other physiological functions (Devinskyet al., 1995). Lesion of the rat medial frontal cortex, includingthe ACC, significantly increased hot-plate latency (Pastorizaet al., 1996). In patients with frontal lobotomies or cingulotomies,the unpleasantness of pain is abolished (Foltz and White, 1962;Hurt and Ballantine, 1973; Yarnitsky et al., 1988; Stanton andSejnowski, 1989; Artola et al., 1990; Stevens, 1990; Davis etal., 1994; Talbot et al., 1995; Craig et al., 1996). Electrophysiologicalrecordings from both animals and humans demonstrate that neuronswithin the ACC respond to noxious stimuli, including nociceptivespecific neurons (animals: Devinsky et al., 1995; Kenshalo etal., 1988; Sikes and Vogt, 1992; Vogt et al., 1979; humans: Hutchisonet al., 1999). Neuroimaging studies further confirm these observationsand show that the ACC, together with other cortical structures,are activated by acute noxious stimuli (Talbot et al., 1991; Vogtet al., 1996; Davis et al., 1997; Derbyshire et al., 1998; Lenzet al., 1998; Paulson et al., 1998; Hutchison et al., 1999). Ourpresent studies using IEG-encoded protein immunostaining techniquesand neuronal plasticity showed that neurons within the ACC couldshow plastic changes to amputation. In the same animals, behavioralhyperalgesia to noxious stimuli was also observed (our unpublishedobservations). Although it is unlikely that changes in synapticplasticity within the ACC alone explain behavioral hyperalgesia,long-lasting changes within the ACC could certainly contributeto various pain-related functional alterations after amputation.In the present study, we did not address potential changes inother cortical and subcortical areas, such as the somatosensorycortex, thalamus, and spinal cord. It is possible that similarplastic changes may occur in these areas as well. Understandingplastic changes within the areas involved in pain transmissionand modulation after amputation could allow us to treat phantompain in human amputees. From a clinical perspective, our studiesprovide a cellular model for studying synaptic mechanisms forphantom pain. These synaptic changes provide a probe to evaluatethe effect of different drugs that could be potentially usefulfor preoperative and postoperative treatment (Jacobson and Chabal,1989; Katz and Melzack, 1990; Richmond et al., 1993; Woolf andChong, 1993).

  FOOTNOTES

Received June 22, 1999; revised Aug. 16, 1999; accepted Aug. 18, 1999.

This work was supported by grants from the McDonnell High Brain Function at Washington University and the National Instituteon Drug Abuse. We want to thank Drs. Joseph Henry Steinbach andJames E. Huettner for their helpfulsuggestions.
Correspondence should be addressed to Min Zhuo, Department of Anesthesiology, Washington University, 660 South Euclid Avenue,St. Louis, MO 63110. E-mail: zhuom{at}morpheus.wustl.edu.

  REFERENCES

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ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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