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The Journal of Neuroscience, November 15, 2002, 22(22):9932-9940
Theta-Frequency Synaptic Potentiation in CA1 In Vitro Distinguishes Cognitively Impaired from Unimpaired Aged Fischer 344 Rats
Geoffrey C. Tombaugh, Wayne B. Rowe, Ana R. Chow, Timothy H. Michael, and Gregory M. Rose Memory Pharmaceuticals Corporation, Montvale, New Jersey 07645
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
Hippocampal-dependent learning and memory deficits have been well documented in aging rodents. The results of several recent studies have suggested that these deficits arise from weakened synaptic plasticity within the hippocampus. In the present study, we examined the relationship between hippocampal long-term potentiation (LTP) in vitro and spatial learning in aged (24-26 months) Fischer 344 rats. We found that LTP induced in the CA1 region using theta-frequency stimulation (5 Hz) is selectively impaired in slices from a subpopulation of aged rats that had shown poor spatial learning in the Morris water maze. LTP at 5 Hz in aged rats that did not show learning deficits was similar to that seen in young (4-6 months) controls. We also found that 5 Hz LTP amplitude strongly correlated with individual learning performance among aged rats. The difference in 5 Hz LTP magnitude among aged rats was not attributable to an altered response to 5 Hz stimulation or to differences in the NMDA receptor-mediated field EPSP. In addition, no performance-related differences in LTP were seen when LTP was induced with 30 or 70 Hz stimulation protocols. Finally, both 5 Hz LTP and spatial learning in learning-impaired rats were enhanced with the selective muscarinic M2 antagonist BIBN-99 (5,11-dihydro-8-chloro-11-[[4-[3-[(2,2-dimethyl-1-oxopentyl)ethylamino]propyl]-1-piperidinyl]acetyl]-6H-pyrido[2,3-b][1,4]benzodiazepin-6-one). These findings reinforce the idea that distinct types of hippocampal LTP offer mechanistic insight into age-associated cognitive decline.
Key words: hippocampus; aging; spatial learning; LTP; memory; NMDA receptor; muscarinic receptor
INTRODUCTION
Learning and memory impairments are among the most commonly recognized psychological features of human aging. In the absence of pathological dementia, however, aging and cognitive decline are not obligatorily linked: some aged individuals exhibit keen learning and memory ability into and beyond their eighth and ninth decades (McClearn, 1997
; Backman et al., 2000
Like humans, aged rodents exhibit a marked heterogeneity in their ability to learn and remember. Spatial learning is particularly impaired in aged rats, but some aged subjects show severe deficits in spatial learning, whereas others are indistinguishable from young controls (Gage et al., 1984
Since its first formal description (Bliss and Lomo, 1973
Numerous stimulation protocols reliably elicit LTP in the hippocampus. However, the utility of these protocols in probing mnemonic mechanisms may not be equal. Diverse stimulus protocols can trigger increases in synaptic responses [e.g., field EPSPs (fEPSPs)] that are similar in amplitude and stability yet arise from different biochemical cascades depending on the pattern of stimulation, age, species, and even strain of the animal (Shankar et al., 1998
Any model that attempts to link hippocampal LTP to hippocampal-based learning generates two key predictions. First, LTP deficits should exist only in learning-impaired subjects and should ideally covary with individual learning ability. Second, pharmacological manipulations that enhance learning should also augment LTP. In the present study, we describe an in vitro LTP protocol that meets both of these criteria.
MATERIALS AND METHODS
Animals. Young (Y) (4-6 months old) and aged (24-26 months old) male Fisher 344 rats were obtained from Hilltop Lab Animals (Scottdale, PA). The animals were left undisturbed for a minimum of 1 month in our facility until the beginning of behavioral testing. Rats were housed in pairs in polycarbonate cages (45 × 30 × 18 cm) with corncob bedding and maintained on a 12 hr light/dark schedule (lights off at 7:00 P.M.). Food (LabDiet 5001 rodent diet; Purina Mills, St. Louis, MO) and water were available ad libitum. Animal health was monitored by a veterinarian; animals showing overt signs of morbidity were removed from the study. All procedures were conducted in accordance with local Institutional Animal Care and Use Committee guidelines.
Behavior. Young and aged rats were tested in the Morris water maze as described previously (Rowe et al., 1998
The cognitive status of the aged animals was defined on the basis of their latencies to find the submerged platform on days 3, 4, and 5 of testing relative to the mean latency of young controls (see Fig. 1). Aged-impaired (AI) rats were defined as those animals whose mean latencies (across the 3 d of testing) differed by >3.0 SDs from that of young controls. Aged animals were considered unimpaired (AU) if their mean latencies were
0.5 SD from young controls. Aged animals whose mean escape latencies fell between these values were not used in any additional tests.
BIBN-99 (5,11-dihydro-8-chloro-11-[[4-[3-[(2,2-dimethyl-1-oxopentyl) ethylamino]propyl]-1-piperidinyl]acetyl]-6H-pyrido[2,3-b][1,4]benzodiazepin-6-one), a selective muscarinic M2 receptor antagonist (Doods et al., 1993a
Slice physiology. Rats were anesthetized with isoflurane and killed by decapitation. Transverse hippocampal slices (400 µm) were prepared from young adult and a subset of behaviorally characterized aged rats using a tissue chopper. Slices were maintained at 28°C in an interface chamber (Fine Science Tools, Foster City, CA) and perfused at 1-2 ml/min with artificial CSF (ACSF) that had been preequilibrated with 95%O2-5%CO2. The ACSF composition was as follows (in mM): 124 NaCl, 4.5 KCl, 1 NaH2PO4, 26 NaHCO3, 2.5 CaCl2, 1.3 MgCl2, and 10 glucose. Bipolar stimulating electrodes (stainless steel; Frederick Haer Co., Bowdoinham, ME) and glass recording electrodes (1-3 M
; filled with ACSF) were positioned in stratum radiatum of area CA1. Input-output curves were recorded, and test stimulus intensity (0.017 Hz, 50 µsec duration) was adjusted to evoke an fEPSP with an initial slope that was 40-45% of maximum. After a stable baseline period (20-30 min), one of three stimulation protocols was applied at the test intensity: (A) a single 30 sec train at 5 Hz; (B) three 0.5 sec trains at 30 Hz (5 min intertrain interval); or (C) three 0.5 sec trains at 70 Hz (5 min intertrain interval). After the induction protocol, single responses were evoked at the test intensity for 50-60 min (A) or 180 min (B and C) to monitor LTP amplitude and stability. LTP was measured by comparing the mean fEPSP slope (averaged over 5 min) at the end of the post-tetanus period with that of the mean fEPSP slope recorded 5 min before either the tetanus or BIBN-99 application. The effect of NMDA receptor (NMDAR) blockade on 5 Hz LTP was examined in slices from young rats by exposing the slices to 50 µM APV for 15 min and sequentially applying 5 Hz stimulation to the same slice, first in the presence of APV and then 60 min later after washout. BIBN-99 was dissolved in DMSO; stock solutions were diluted in ACSF immediately before use and bath applied to slices 30 min before LTP induction at a final concentration of 1.0 µM. The DMSO concentration never exceeded 0.05%. NMDA receptor-mediated fEPSPs were isolated by exposing slices for 50-60 min to modified ACSF containing 200 µM MgCl2, 10 µM CNQX, and 10 µM glycine.
Slices from aged rats subjected to 5 or 30 Hz stimulation were prepared from different hippocampi of the same rat; experimenters were blind to the behavioral status of the animal. Slices subjected to 70 Hz stimulation were taken from a separate group of rats. In all cases, recordings from young and aged slices were interleaved. Recordings on a given day were typically made from multiple slices (two to four) from each animal. For LTP behavior correlations and NMDAR fEPSP measures, the datum for a given animal was represented by the average value from all slices examined. In experiments in which BIBN-99 was applied, paired control recordings were always performed in adjacent slices from the same animal. Complex spiking observed during 5 Hz stimulation was quantified by counting the number of negative spikes clearly resolved from the fEPSP (Thomas et al., 1998
RESULTS
Learning impairments can be observed in a subset of aged rats
Aged rats were characterized as either AI or AU based on their mean escape latency derived from training days 3-5 in the Morris water maze. As anticipated from previous studies, aged rats showed significantly longer swim times and swim distances with a greatly increased variance compared with young controls. Aged rats swam more slowly than young rats (young, 27.9 ± 0.6 cm/sec; AU, 24.9 ± 0.4 cm/sec; AI, 23.1 ± 0.5 cm/sec). Importantly, there was no significant difference in swim speed between AU and AI animals. Swim times and distances were highly correlated for all groups (r > 0.9 in all cases).
Swim times for aged rats exhibited a skewed, unimodal distribution (Fig. 1A). Of 89 aged animals screened in the water maze for the present study, 40 (45%) were classified as AI, and 21 (24%) were classified as AU (see Materials and Methods). The remainder of the animals did not fall clearly into either category and were excluded from additional study. The acquisition curves for the AU and AI groups illustrate the dramatic impairment in the ability of AI animals to find the hidden platform (Fig. 1B,C). However, when the platform was made visible, all young and AU and all but four AI rats were able to achieve criterion performance (see Materials and Methods). The mean swim times for young, AU, and AI rats that reached criterion in the visually cued trials were 5.0 ± 0.3, 8.5 ± 1.0, and 8.8 ± 0.8 sec, respectively. These data suggest that the altered ability of the AI animals to locate the submerged platform was not attributable to a visual, motor, or motivational deficit.
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Figure 1. Morris water maze testing reveals a broad gradient of learning ability among aged F344 rats. A, Mean escape latencies measured on training days 3-5 were grouped in 10 sec bins for both aged (24-26 months) and young (4-6 months) rats. AU or AI animals were identified as those whose mean performance differed by <0.5 or >3 SDs from the mean of young controls, respectively. The remaining rats [aged-other (AO)] were excluded from additional study. The acquisition curves during training are plotted for both mean escape latency (B) and path length (C). Error bars in B and C, when not visible, are smaller than the symbol size.
AI rats do not use a spatial strategy in the water maze
At the end of the 5 d training period, each animal was given a 30 sec probe test, during which the submerged escape platform was unavailable. The swim speeds of AU and AI rats did not differ during the probe trial (AU, 23.9 ± 0.6 cm/sec; AI, 23.4 ± 0.4 cm/sec) and were comparable with that of young controls (25.4 ± 0.5 cm/sec). However, AI animals required significantly more time to make their first entry into the annulus-40 compared with either AU or young rats (p < 0.05; ANOVA) (Fig. 2A). The AI rats also maintained a significantly greater mean distance from the platform during the probe trial (p < 0.05; ANOVA; data not shown). Young and AU rats had nearly identical first entry latencies (Fig. 2B).
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Figure 2. Probe measures indicate that AI rats do not use a spatial strategy in the water maze. A, Schematic of the water maze. B, With the platform removed, AI rats required significantly more time for their first entry into the annulus-40 than AU or young rats. AI and AU data were derived from animals used for subsequent electrophysiological analysis in Figures 4 and 5 (Y, n = 36; AU, n = 7; AI, n = 13). *p < 0.05 compared with AU group. C, AI rats spent less time within the target area than AU or Y rats. Dwell time for AI rats (dashed line), unlike that for AU and Y rats, was unchanged when the extramaze cues were obscured by a curtain (Y, n = 12; AU, n = 11; AI, n = 11). **p < 0.01 and ***p < 0.001 compared with matching "no curtain" control (paired t test). #p < 0.05 and $p < 0.05 compared with Y and AU no curtain groups, respectively (unpaired t test).
Consistent with the first-entry data, AI rats spent significantly less time (1.32 ± 0.5 sec) swimming in the annulus-40 than either AU (3.1 ± 0.7 sec; p < 0.05) or young (6.8 ± 0.7 sec; p < 0.001) rats. Surprisingly, the dwell time for AU rats was also significantly smaller than young controls (p < 0.01; ANOVA). This finding suggested that AU rats may have used a distinct (i.e., nonspatial) strategy to locate the platform and prompted us to examine this question in more detail. New groups of identically trained animals were subjected to a revised probe analysis in which a curtain was placed around the pool to obscure the extramaze cues (Fig. 2C). No-curtain dwell times in all groups were nearly identical to those seen in the first study. With the curtain present, however, dwell times for young and AU rats fell to the level seen in AI rats, whereas the dwell time for the AI rats was unchanged.
BIBN-99 improves spatial learning in AI rats
Based on previous studies (Quirion et al., 1995
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Figure 3. BIBN-99 improves water maze performance in AI rats. The mean escape latency (A) and latency to first entry into the annulus-40 (B) were reduced, whereas dwell time in the annulus-40 (C) was significantly increased after a single injection of BIBN-99 given 45 min before each set of training trails over 3 d. Baseline data refer to those collected on training days 3-5 for rats that received either vehicle (n = 8) or BIBN-99 (n = 11) injections on days 6-8. *p < 0.01 compared with pretreatment baseline (paired t test).
Slices from young and aged rats respond similarly to electrical stimulation
Input-output (stimulus-response) curves were generated from slices from Y AU and AI rats by plotting the fEPSP slope as a function of fiber volley amplitude. For a given fiber volley amplitude, evoked responses from aged slices were consistently smaller than those from young controls (Fig. 4A). However, input-output curves for AU and AI animals were not statistically different. In addition, no significant difference in paired-pulse facilitation was observed among the groups across a range of interstimulus intervals (Fig. 4B).
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Figure 4. Slices from AU and AI rats exhibit no differences in CA1 synaptic transmission and short-term facilitation. A, Input-output curves reveal depressed synaptic transmission for aged rats relative to young controls but were not different between AU and AI subgroups [Y, n = 9(7); AU, n = 9(7); AI, n = 19(8)]. B, Paired-pulse facilitation in CA1 was indistinguishable between young, AU, and AI groups across a range of interstimulus intervals (ISI). Inset shows a representative trace (young rat). Calibration: 2 mV, 10 msec.
Theta-frequency stimulation in vitro reveals an LTP deficit in AI rats
Thirty seconds of 5 Hz stimulation routinely induced robust LTP in slices taken from young rats. This form of potentiation rose gradually and stabilized within 10-15 min after the 5 Hz train (Fig. 5A). LTP in slices from AU rats was comparable with that seen in young animals, but LTP elicited from AI slices was significantly smaller (p < 0.001; ANOVA) (Fig. 5A). During 5 Hz stimulation, complex spiking gradually emerged and was observed in all three groups (Fig. 5B). No dramatic differences were seen in the average latency to spiking, as measured by the stimulus number at which one-half of the slices experienced the first spike (Y, 54; AU, 50; AI, 53). We also found no difference in the total number of spikes evoked (Y, 131 ± 10; AU, 120 ± 11; AI, 131 ± 18).
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Figure 5. LTP at 5 Hz distinguishes between slices from AI and AU rats. A, AI slices subjected to 5 Hz, 30 sec stimulation exhibited significantly smaller synaptic potentiation in CA1 than that seen in either young or AU slices [Y, n = 17(8); AU, n = 20(7); AI, n = 32(13)]. ***p < 0.001 compared with young and AU. B, All groups responded to 5 Hz stimulation with a similar time course and number of complex spikes. Inset in B shows a representative set of traces collected during 30 sec of 5 Hz stimulation in a young slice. Calibration: 1 mV, 10 msec. C, Slices taken from the contralateral hippocampus of a subset of animals in A were subjected to three 0.5 sec trains at 30 Hz stimulation. The resulting LTP in both AU and AI slices was smaller than that in young controls (p < 0.05), but no AU-AI difference was detected [Y, n = 17(14); AU, n = 11(6); AI, n = 8(5)]. D, Stimulation at 70 Hz in a separate set of rats induced robust, long-lasting, and statistically equivalent LTP in all groups [Y, n = 13(11); AU, n = 17(9); AI, n = 8(7)]. Data points in C and D are presented at 5 min intervals for clarity.
To determine whether the depressed LTP observed in AI rats was a function of the 5 Hz stimulation protocol, parallel experiments were run in which higher-frequency stimulation was applied to slices taken from the opposite hippocampus of the same animals. In these slices, LTP was induced with three 0.5 sec trains of 30 Hz stimulation, with a 5 min intertrain interval (Fig. 5C). Under these conditions, LTP amplitude at 3 hr was significantly reduced in both AU and AI rats (p < 0.05) compared with young controls, but no statistically significant AU-AI difference emerged. In slices from a separate set of animals, increasing the stimulation frequency to 70 Hz generated a more robust but equivalent level of LTP in all three groups (Fig. 5D).
LTP deficits in AI rats do not arise from reduced NMDA receptor function
LTP at 5 Hz in adult mice has been shown previously to be partially NMDA receptor dependent (Thomas et al., 1998
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Figure 6. The deficit in 5 Hz LTP in AI rats is not linked to a loss of NMDA receptor function. A, LTP at 5 Hz in young slices [n = 7(4)] is partially NMDA receptor dependent, because bath application of 50 µM APV (hatched bar) depressed but did not completely block LTP triggered by 5 Hz, 30 sec stimulation ( ). Insets depict the 1st and 150th sweeps recorded from the same slice during the two successive 5 Hz trains. Complex spiking during 5 Hz stimulation in the presence of APV was abolished. After washout, 5 Hz stimulation triggered complex spiking (total spikes, 98 ± 12) and robust LTP that was comparable with that typically seen in naïve control slices (see Fig. 5). B, The NMDA receptor-mediated fEPSP, isolated in the presence of 10 µM CNQX, 10 µM glycine, and 0.2 mM Mg2+ was depressed in both AU and AI rats by ~30% compared with young controls across a range of stimulus intensities [Y, n = 21(7); AU, n = 18(6); AI, n = 13(6)]. When normalized to fiber volley amplitudes >0.5 mV, slope values for both AU and AI rats were significantly different from young controls (p < 0.01). No difference between AU and AI rats was detected. Inset depicts representative traces (average of 5 sweeps) recorded from an aged rat slice before and after exposure to 50 µM APV. Calibration: 1 mV, 10 msec.
LTP at 5 Hz correlates with performance in the Morris water maze
To further explore the possible link between 5 Hz LTP and spatial learning, we plotted LTP amplitude, measured at 1 hr after LTP induction, against three behavioral measures (Fig. 7). Regression analysis revealed a strong negative correlation between 5 Hz LTP and mean escape latency among aged rats (p < 0.001) (Fig. 7A). LTP at 5 Hz was also highly correlated with two measures of probe trial performance: (1) latency to the first entry into the annulus-40 (p < 0.05) (Fig. 7B); and (2) cumulative dwell time in the annulus-40 (p < 0.01) (Fig. 7C).
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Figure 7. LTP at 5 Hz correlates with water maze learning in aged rats. A, The average level of 5 Hz LTP calculated for each aged animal was strongly correlated to individual mean escape latency in the water maze (A; R2 = 0.50; p < 0.001). In addition, 5 Hz LTP was significantly correlated to two probe measures: the latency to first entry into the annulus-40 (B; R2 = 0.24; p < 0.05) and total dwell time in the annulus-40 (C; R2 = 0.42; p < 0.01). In each case, the data for young control rats are presented for comparative purposes only and were not included in the regression analysis.
BIBN-99 enhances 5 Hz LTP
Given that BIBN-99 improved water maze performance in AI rats, we tested the possible link between 5 Hz LTP and spatial learning by asking whether BIBN-99 could also enhance 5 Hz LTP. Bath application of 1 µM BIBN-99 to AI slices for 30 min had no observable effects on baseline responses either during drug delivery or 60 min after washout [104 ± 4%; n = 5(2)]. In contrast, BIBN-99 significantly enhanced the degree of synaptic potentiation in AI slices after 5 Hz stimulation (p < 0.001) (Fig. 8A). This action was probably unrelated to any direct potentiating effect on the NMDA receptor itself, because a 30 min application of 1 µM BIBN-99 did not alter the slope of the isolated NMDA fEPSP recorded in AI slices (103 ± 2% of baseline; n = 6). In addition, BIBN-99 did not change the onset or total number of complex spikes evoked during the 5 Hz train (Fig. 8B). In contrast to its effect on 5 Hz LTP, BIBN-99 (1 µM) failed to enhance LTP in AI slices evoked by repeated 70 Hz trains (Fig. 8C). Finally, the same concentration of BIBN-99 did not modify 5 Hz LTP recorded in slices from young rats (control, 152 ± 8%; BIBN-99, 144 ± 7%).
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Figure 8. BIBN-99 enhances 5 Hz LTP in slices from AI rats. A, Bath application of 1 µM BIBN-99 (thick bar) significantly enhanced 5 Hz LTP in AI slices [n = 9(5)] to a level slightly smaller than that seen in young controls [n = 17(8)]. ***p < 0.001, AI plus BIBN-99 compared with AI control. B, BIBN-99 did not significantly affect the time course or total number of complex spikes evoked during 5 Hz stimulation. C, BIBN-99 had no effect on LTP evoked by repeated trains of 70 Hz stimulation in AI slices (see Materials and Methods). Data points in C are presented at 5 min intervals for clarity. Error bars were smaller than the symbol size.
DISCUSSION
The key findings in this study are that a specific form of hippocampal LTP in aged rats evoked by theta-frequency stimulation (1) strongly correlates with individual performance on a spatial learning task and (2) can be amplified by a selective muscarinic M2 antagonist that also improves spatial learning.
One critical element in this study that enabled us to examine the linkage between LTP and learning was our ability to distinguish learning-impaired from unimpaired aged rats. Although our definition of "impaired" is statistically based and not absolute, this approach helped create more uniform experimental groups and removed aging per se as a variable. Compared with young rats, aged rats exhibited a right-shifted, broadly skewed gradient of water maze performance (escape latency). This distribution appeared unimodal, suggesting that both AU and AI animals were members of the same population, as might be expected for the inbred Fischer 344 (F344) strain. Thus, age-related cognitive decline in the rat, although often observed, is not an inevitable consequence of aging.
After the 5 d training period, probe trial analysis showed that both young and AU rats entered the annulus-40 with the same latency, suggesting an equivalent certainty of the platform location. Surprisingly, the AU rats spent significantly less time in the annulus-40 with fewer platform crossings (data not shown) than young rats during the probe trial. This difference in perseverance suggests that AU rats either (1) recognized that the platform was absent and adapted by deliberately searching elsewhere or (2) grew less certain about the platform location and swam randomly. We are currently unable to distinguish between these two possibilities. Although AU and Y rats perform similarly in the water maze, they are not identical in all measures and thus cannot be viewed as equivalent. However, the critical fact remains that both Y and AU rats were clearly dependent on extramaze cues and thus, unlike AI rats, used a spatial (i.e., hippocampus dependent) strategy to solve the task.
Changes in hippocampal synaptic function have been associated previously with age-related memory loss (Barnes, 1994
Hippocampal NMDAR expression is required for normal spatial learning in young rats and mice (Tsien et al., 1996
Our in vitro experiments highlight the ability of 5 Hz, but not 30 or 70 Hz, stimulation to generate a form of LTP that distinguishes AU from AI rats. A general assumption we made is that a change in synaptic efficacy is required for hippocampal-based learning and that these two processes are driven by an overlapping set of cellular mechanisms. A unique consequence of orthodromic theta-frequency stimulation in CA1 is the gradual induction of synchronized complex burst firing in the pyramidal cells. These complex spikes mimic the firing pattern of CA1 neurons in vivo (Kandel and Spencer, 1961
Putative mechanisms for theta-frequency LTP have been described previously (Blitzer et al., 1995
We found that BIBN-99 enhanced spatial learning in AI F344 rats, confirming and extending the results of previous studies that used other rat strains (Pike and Hamm, 1995
How might M2 blockade influence 5 Hz LTP? M2 receptors in the CNS are thought to exist primarily, although not exclusively, as inhibitory presynaptic autoreceptors (Levey et al., 1991
If the relevant consequence of M2 blockade in our study was to elevate synaptic ACh levels, cholinesterase blockade should also enhance 5 Hz LTP. However, we found that the clinically prescribed AChE inhibitor donepezil (Aricept; Eisai, Tokyo, Japan) had no effect on 5 Hz LTP in AI slices when applied at either 1 or 10 µM (data not shown). This negative finding is not likely attributable to the absence of AChE itself (Zhang et al., 1997
The vast majority of M2 receptors in the hippocampus reside as heteroreceptors on GABAergic terminals (Rouse et al., 2000
We chose to examine BIBN-99 in our LTP paradigm because it provided a useful tool to test the putative linkage between spatial learning and LTP. Although muscarinic agents are commonly used to investigate cognitive mechanisms, our results with BIBN-99 do not necessarily suggest a privileged role for cholinergic mechanisms in learning and memory. In fact, ongoing studies in our laboratory have shown that M2 antagonism is not the only route by which 5 Hz LTP and spatial learning can be enhanced. Identifying the key biochemical pathways relevant to both LTP and mnemonic processes remains a large challenge. Our findings illustrate how one can exploit LTP as a tool for identifying learning-memory mechanisms without requiring a detailed understanding of LTP itself.
FOOTNOTES Received May 23, 2002; revised Aug. 23, 2002; accepted Aug. 29, 2002.
We are grateful to Crista Trippodi for help with the statistical analysis and Heather Bimonte for suggesting the curtain experiment.
Correspondence should be addressed to Dr. Geoffrey C. Tombaugh, Memory Pharmaceuticals Corporation, 100 Philips Parkway, Montvale, NJ 07645. E-mail: tombaugh{at}memorypharma.com.
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