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The Journal of Neuroscience, May 21, 2008, 28(21):5513-5518; doi:10.1523/JNEUROSCI.5374-07.2008
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Behavioral/Systems/Cognitive
Visual–Procedural Memory Consolidation during Sleep Blocked by Glutamatergic Receptor Antagonists
Steffen Gais, Björn Rasch, Ullrich Wagner, andJan Born Department of Neuroendocrinology, University of Lübeck, 23538 Lübeck, Germany
Abstract
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Abstract
Introduction
Visual cortex plasticity is enhanced by sleep. It is hypothesized that a reactivation of glutamatergic synapses is essential for this form of plasticity to occur after learning. To test this hypothesis, human subjects practiced a visual texture discrimination skill known to require post-training sleep for improvements to occur. During sleep, glutamatergic transmission was inhibited by administration of the two glutamate antagonists, caroverine and ketamine, targeting the ionotropic NMDA and AMPA receptors. Both substances given during consolidation sleep in a placebo controlled crossover design were able to prevent improvement of the skill measured the next morning. An off-line activation of glutamatergic synapses therefore seems to play a critical part in the consolidation of plastic changes in the visual cortex.
Key words: sleep; memory consolidation; skill learning; visual discrimination; glutamate receptor; human
Introduction
The role of sleep for the development of stable, experience-dependent changes in the visual cortex has been described previously in a number of studies (Karni and Sagi, 1993; Karni et al., 1994
A major hypothesis in sleep and memory research is that those networks that were involved in previous daytime experience are reactivated during sleep (Buzsáki, 1998
Glutamate is one of the main excitatory neurotransmitters in the visual cortex (Baughman and Gilbert, 1980
Memory undergoes a postlearning period of consolidation. If this process is solely dependent on activation during practice, with later maturation depending only on intracellular signaling cascades, it should be independent of intervening synaptic activity. If, however, consolidation depends on reactivation of memory traces, then a temporary blockade of glutamate receptors after learning could prevent post-training memory enhancement (Ribeiro et al., 2004
Materials and Methods
Subjects and general procedure. Two groups of subjects (n = 11 for caroverine; n = 15 for ketamine) participated in the experiments. Subjects were nonsmoking males with normal or corrected to normal vision (age, 24.9 ± 0.8; mean ± SEM). They were screened for acute and chronic diseases, mental disorders, and drug addictions, and they were not taking any medication at the time of the experiments. All of them were normal sleepers (7–9 h per night) with no major disruptions of the sleep–wake cycle during the 6 weeks before the experiments. Subjects were not allowed to take in caffeine and alcohol or to sleep during daytime before experimental nights.Before the experiments, subjects were accustomed to sleeping under laboratory conditions. Each subject participated in two experimental sessions (substance and placebo), which followed a double-blind, randomized, and balanced crossover design. Sessions were spaced at least 4 weeks apart. On the days of the experiments, subjects learned the visual texture discrimination task (VDT) at 10:00 P.M. At
11:00 P.M. they went to bed and lights were turned off. Substance administration started at sleep onset, defined by the first occurrence of sleep stage 2. Subjects were awakened 8 h after sleep onset. Retesting took place 30 min after awakening (see Fig. 1b). Sleep was recorded polysomnographically and scored according to standard criteria. Aside from retrieval testing, testing after sleep included an assessment of subjective tiredness by questionnaire as well as an interview regarding side effects of substance administration. Statistics generally relied on an ANOVA with the two within-subject factors pretest/post-test and substance/placebo. Experiments were approved by the Ethics Committee of the University of Lübeck.
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Figure 1. VDT. a, Task: stimulus (left) and mask (right) as used in the visual discrimination task. The letter in the center of the stimulus serves to ensure proper fixation. The target (oblique bars) is thus perceived only peripherally. It appears always in the same quadrant, but quadrants were changed between substance conditions. The subject is required to discriminate whether the bars are aligned horizontally (as in this example) or vertically. The mask follows the stimulus after an SOA of 20–300 ms to extinguish afterimages of the stimulus. b, Illustration of how actual detection thresholds were determined. c, Experimental design: two different groups of subjects (Exp. 1, Exp. 2) each participated in two conditions, receiving substance (caroverine, 80 mg, or ketamine, 0.6 mg/kg body weight) and placebo according to a balanced crossover design. Substance infusion started at sleep onset and continued for 6 h. d, VDT performance: mean (±SEM) detection thresholds of subjects during pretest before sleep (gray bars) and post-test after sleep (white bars). During sleep between tests subjects received placebo, caroverine (top), or ketamine (bottom). In both placebo conditions, subjects showed significantly lower discrimination thresholds and, thus, a better performance, at post-test after sleep. In both substance conditions, no such increase in performance through learning was achieved. Pretest/post-test by placebo/substance interactions are significant. *p < 0.05.
Behavioral testing. All tests took place in a soundproof, dark chamber. Subjects in the main experiments had to learn a VDT, which required them to discriminate between a small horizontal or vertical target stimulus, presented briefly in the periphery of the visual field (Karni and Sagi, 1991Before the experiment proper, subjects practiced the task in the presence of the experimenter with 50 additional trials at an SOA of 400 ms. The stimuli were 16° of visual angle in size and consisted of a 19 x 19 field of horizontal bars (17 x 17 cm) with a randomly rotated T- or L-shaped figure in the center. Bars were 0.6° (6 mm) long and 0.05° (0.4 mm) wide. Stimuli had an intensity of 2.25 cd/m2, background intensity was 0.01 cd/m2. The pop-out target was located at a distance of 3–5° visual angle from the center and consisted of three oblique bars aligned either horizontally or vertically. The target was shown in the same quadrant of the visual field during learning and subsequent retrieval, but in different quadrants for the two experimental conditions, because learning in this task is restricted to the retinal position where the target appeared. After each trial the subject had to press one of two keys to indicate which letter had been presented in the center of the screen to ensure proper fixation, and whether the target was aligned horizontally or vertically. Errors on the fixation task were indicated instantly by a tone. All subjects met the criterion of >90% correct responses in the T/L discrimination until at least 1 step below the discrimination threshold for the horizontal/vertical discrimination (on average, 98.1% correct in the block directly above threshold SOA for the horizontal/vertical task). Only trials with a correct response entered into the analysis, thus excluding all trials with an obvious lack of fixation, but leaving those trials with improper fixation where the subjects guessed the correct response (i.e., statistically half of the fixation errors were omitted from analysis). Because of the small number of fixation errors, these can be expected to have only a minor effect on the analysis. There was no time limit for giving the answer, and subjects were told to take breaks when needed. Performance was measured with reference to the per cent correct responses at a given SOA. Threshold SOA was calculated by interpolating the SOA with a recognition rate of 80%. The detection threshold for fixation stimuli was also calculated using the same method. The procedure for retrieval testing was identical to that used during the learning session.
Substance administration and blood sampling. Thirty minutes before behavioral testing, two intravenous catheters were inserted into the subject's forearm for blood sampling and substance administration. Beginning with sleep onset, subjects received in the verum condition a slow, constant intravenous infusion of 50 ml of isotonic saline solution with either 0.25 mg/kg body weight of S-ketamine (Ketanest S; Pfizer) or 80 mg of caroverine (Calmaverine; Taphlan) over 6 h. Placebo was 50 ml of isotonic saline solution. Both substances are acting predominantly as glutamate receptor antagonists. Ketamine is an NMDA receptor antagonist and has been used in high doses primarily for this action as local or general anesthetic. Previously, it has been proposed that ketamine might also bind to dopaminergic D2 receptors (Kapur and Seeman, 2002
To control for neuroendocrine side effects, blood was collected during sleep via thin plastic tubes from an adjacent room without disturbing subjects' sleep. Blood was sampled before and after test performance and hourly, beginning 30 min after sleep onset. Blood was immediately centrifuged and frozen at –20°C until assay. Cortisol was determined from serum by enzyme immunoassay (DSL-10-2000 Active Cortisol; Diagnostic Systems Laboratories). Blood norepinephrine levels were determined from EDTA-plasma by standard high-performance liquid chromatography (Waters) with electrochemical detection.
Results
In a first experiment, we administered the AMPA receptor antagonist caroverine during sleep after subjects had practiced a VDT, which required subjects to determine the direction of a target stimulus displayed only for a very brief interval (Gais et al., 2000Sleep was recorded during the night after task practice. Sleep-stage distribution and total sleep time were comparable between caroverine and placebo conditions (Table 1). Measures of cortisol and norepinephrine were also taken throughout the night. Total secretion [area under curve (AUC)], minimum (Min), and maximum (Max) values did not differ between both conditions [placebo vs caroverine, p > 0.20 for all comparisons; cortisol: AUC (in µg*h/dl) 71.9 ± 7.9 vs 68.2 ± 7.5, Min (in µg/dl) 1.7 ± 0.5 vs 1.7 ± 0.4, Max (in µg/dl) 19.6 ± 1.0 vs 19.8 ± 1.0; norepinephrine: AUC (in pg*h/ml) 1302 ± 114 vs 1284 ± 88, Min (in pg/ml) 95 ± 9 vs 86 ± 11, Max (in pg/ml) 310 ± 34 vs 329 ± 29].
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Table 1. Sleep stage distribution and total sleep time during experimental and control conditions of the experiments testing visual texture discrimination learning
In the second experiment, the NMDA receptor antagonist ketamine was administered according to the same experimental design used in the first experiment. Healthy subjects received ketamine during sleep after practice of the VDT. The results showed a pattern similar to that of caroverine administration. There was no significant improvement in performance between pretest and post-test if subjects received ketamine (t(14) = –0.38; p = 0.71) (Fig. 1c). When subjects received placebo, they showed the known postlearning amelioration of discrimination performance (t(14) = 2.2; p = 0.04). The decrease in detection thresholds with reference to training before sleep averaged –14.7 ± 6.6 ms after placebo, whereas after ketamine detection thresholds slightly increased by +1.5 ± 4.3 ms on average. Comparing both conditions revealed a significant measurement by substance interaction (F(1,14) = 4.9; p = 0.04).Sleep was not affected by ketamine (Table 1). Total secretion, minimum, and maximum values of cortisol and norepinephrine did not show differences between conditions [placebo vs ketamine, p > 0.55 for all comparisons; cortisol: AUC (in µg*h/dl) 70.2 ± 4.8 vs 72.7 ± 3.6, Min (in µg/dl) 1.4 ± 0.1 vs 1.4 ± 0.1, Max (in µg/dl) 19.3 ± 0.6 vs 18.8 ± 0.7; norepinephrine: AUC (in pg*h/ml) 1486 ± 121 vs 1497 ± 112, Min (in pg/ml) 85 ± 13 vs 84 ± 6, Max (in pg/ml) 529 ± 49 vs 492 ± 51].
In both experiments, no significant differences between placebo and substance conditions were found for subjective ratings of tiredness and concentration (p > 0.55). The detection threshold for the fixation stimuli during VDT performance also did not differ between placebo and substance (placebo vs ketamine, 67.2 ± 6.4 ms vs 69.4 ± 6.8 ms, p > 0.49; placebo vs caroverine, 74.3 ± 5.3 ms vs 72.3 ± 4.1 ms, p > 0.59), indicating comparable vigilance in both conditions and excluding unspecific effects of the substances on the visual system. Subjects were unable to guess above chance level in which condition they received the active substance.
Discussion
Research in recent years showed that knowledge about memory systems can be gained by looking at what happens to memory during sleep. For the VDT used in the present experiments, it is known that training related improvements occur only across subsequent periods of sleep (Gais et al., 2000The requirement of glutamate receptor activation during consolidation of the VDT fits well into the theoretical framework of memory trace reactivation underlying off-line enhancements in memory. Information in the visual cortex is transmitted via NMDA- and AMPA-type glutamate receptors (Rivadulla et al., 2001
Synapse reactivation might serve different purposes. Synaptic potentiation induced during previous learning would decay within hours if it is not stabilized at a later point (Frey and Morris, 1997
Several other studies looked also at postlearning administration of glutamatergic antagonists (Riedel et al., 2003
Footnotes
Received Dec. 5, 2007; revised March 11, 2008; accepted April 4, 2008.This work was supported by Deutsche Forschungsgemeinschaft SFB 654.
Correspondence should be addressed to either Jan Born or Steffen Gais, Department of Neuroendocrinology, University of Lübeck, Ratzeburger Allee 160, 23538 Lübeck, Germany. Email: born{at}kfg.uni-luebeck.de or Email: gais{at}kfg.uni-luebeck.de
Copyright © 2008 Society for Neuroscience 0270-6474/08/285513-06$15.00/0
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