1 Department of Psychology and The Centre for Neuroscience, University of Otago, Dunedin, New Zealand; and 2 Department of Psychology, Princeton University, Princeton, New Jersey 08544
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ABSTRACT |
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Colombo, Michael, Tom Fernandez, Katsuki Nakamura, and Charles G. Gross. Functional differentiation along the anterior-posterior axis of the hippocampus in monkeys. J. Neurophysiol. 80: 1002-1005, 1998. We tested whether the primate hippocampus was functionally heterogenous along its anterior-posterior axis. Two monkeys were trained on both a spatial and nonspatial memory task and the incidence of spatial and nonspatial delay activity in the anterior, middle, and posterior hippocampus was noted. Spatial delay activity (activity in the delay period after the sample stimulus on the spatial memory task) was more common in the posterior than the anterior hippocampus, whereas nonspatial delay activity (activity in the delay period after the sample stimulus on the nonspatial memory task) was evenly distributed throughout the hippocampus. Furthermore, delay neurons in the anterior hippocampus exhibited scalloping delay activity, whereas those in the middle and posterior hippocampus did not. These findings suggest that the hippocampus is functionally heterogeneous and that the posterior regions may be more important for processing spatial information, whereas the anterior regions may be more important for directing or coding movements to points in space.
A review of the hippocampal literature reveals a range of impairments that are difficult to collapse under the umbrella of a single theory. For example, views that the hippocampus is only critical for memory (Eichenbaum et al. 1994 Two monkeys (Macaca fascicularis) were trained on both spatial and nonspatial delayed matching-to-sample (DMS) tasks. The stimulus for the spatial DMS task consisted of a 16-lobed pattern, whereas the stimuli for the nonspatial DMS task consisted of a picture of a monkey face and a 4-lobed pattern. The DMS procedure was identical for both tasks. At the end of a 10-s intertrial interval (ITI), a high-frequency tone was presented for 0.2 s, followed by the presentation of a sample stimulus for 1 s on either the left or right side of the monitor. The sample stimulus was then turned off and a 5-s delay period followed. At the end of the delay period, two comparison stimuli were presented for 2 s, one on the right side and the other on the left side of the monitor. A response to the correct comparison stimulus resulted in a reward (cranberry juice), followed by the ITI. A response to the incorrect comparison stimulus, or failing to press within the 2-s response window, resulted in a 10-s time-out period, which was then followed by the ITI.
Coronal reconstructions of the electrode tracks are shown in Fig. 1. For both monkeys there were three main clusters of electrode tracks positioned within or aimed in the direction of the anterior (A12.4 and A12.3), middle (A9 and A9.7), and posterior (A4.7 and A5.1) hippocampus. Of the 94 neurons sampled, 41 (43.6%) exhibited delay activity, a number similar to that reported in a previous study (Colombo and Gross 1994
Two main findings emerged from the current study. First, spatial delay activity was predominantly located in the posterior rather than the anterior hippocampus, whereas nonspatial delay activity was evenly distributed throughout the hippocampus. Second, scalloping delay activity was noted in the anterior rather than the middle and posterior hippocampus.
INTRODUCTION
Abstract
Introduction
Methods
Results
Discussion
References
; Squire 1992
) or cognitive mapping (O'Keefe and Nadel 1978
) often fail to consider the well-documented nonmnemonic and nonspatial impairments that follow hippocampal lesions (Gray and McNaughton 1983
) as well as the many findings that hippocampal unit activity is modulated by movement-related factors (Foster et al. 1989
; Sharp et al. 1995
).
; Moser et al. 1993
), and there has been suggestive evidence that the same may be true in primates (Colombo and Gross 1994
, 1996
; Watanabe and Nike 1985). These findings raise the possibility that the hippocampus may be functionally heterogenous and that different functions may fall under the jurisdiction of different regions within the hippocampus. The goal of the current experiment was to test for functional differentiation within the primate hippocampus. In particular, we examined whether the posterior hippocampus in monkeys, which is considered equivalent to the dorsal hippocampus in rats (Witter 1993
; Witter and Amaral 1991
), was more important for processing spatial information than the anterior hippocampus.
METHODS
Abstract
Introduction
Methods
Results
Discussion
References
). Extracellular activity of single isolated neurons was recorded by using tungsten microelectrodes.
). We compared the percentage of neurons displaying spatial and nonspatial delay activity across these areas. A delay neuron is a neuron that fires more (or less) during the delay period of a DMS task than during the ITI (baseline) period. A number of investigators have suggested that delay activity represents a neural correlate of memory (Colombo and Gross 1994
; Funahashi et al. 1989
; Fuster and Jervey 1982
; Miyashita and Chang 1988
).
RESULTS
Abstract
Introduction
Methods
Results
Discussion
References
). Of these 41 delay neurons, 15 responded exclusively in the delay period after the spatial stimulus, 3 responded exclusively after the nonspatial face stimulus, and 2 responded exclusively after the nonspatial pattern stimulus. The remaining 21 delay neurons all responded in the delay period after the spatial stimulus and to either one or both of the nonspatial stimuli.
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FIG. 1.
Coronal reconstructions of the anterior, middle, and posterior recording sites for the 2 monkeys.
). The relationship between sample activity and delay activity was again examined in the current study. Delay activity was considered to be related to sample activity if, for example, a neuron fired significantly during the delay period and the presentation of the sample stimulus. In line with our previous findings, there were approximately an equal number of sample-dependent and sample-independent instances of delay activity; this was the case for spatial (50 vs. 50%), nonspatial face (55.6 vs. 44.4%), and nonspatial pattern (52.4 vs. 47.6%) delay activity.
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FIG. 2.
Distribution of spatial and nonspatial delay activity across the anterior (A), middle (M), and posterior (P) regions of the hippocampus.
) we noticed that delay neurons in anterior hippocampus exhibited scalloping activity; that is, the magnitude of the delay activity increased as the delay progressed. Some researchers have suggested that scalloping delay activity may represent a neural correlate of an imminent response (Fuster 1993
; Halgren 1991
). Given that hippocampal unit activity can be modulated by movement-related factors (Foster et al. 1989
; Sharp et al. 1995
), we were interested in whether there were any regional differences in the expression of scalloping activity by hippocampal delay neurons. Delay activity across the 5-s delay period was collapsed into 1-s bins and plotted as a change in activity compared with the ITI (baseline) activity level. Owing to the small number of excitatory delay neurons (n = 12), we restricted this analysis to inhibitory delay neurons (n = 29). The results are shown in Fig. 3. Repeated-measures analysis of variance conducted on both the spatial and nonspatial delay activity data with position (3: anterior vs. middle vs. posterior) and delay period (5: bins 1-5) as factors revealed a significant position × delay period interaction effect both for neurons displaying spatial delay activity [F(8, 92) = 3.21, P < 0.01] and nonspatial delay activity [F(8, 108) = 4.11, P < 0.01]. Separate univariate tests showed that only for the anterior spatial delay activity [F(4, 20) = 4.57, P < 0.01] and the anterior nonspatial delay activity [F(4, 32) = 5.08, P < 0.01] was there a significant decrease in activity (i.e., became more inhibitory) across the 5-s delay period. In contrast, there was no evidence that the magnitude of delay activity varied across the delay period for either spatial or nonspatial delay activity in the middle or posterior hippocampus (all Ps > 0.07). Thus scalloping delay activity was a feature of delay neurons in the anterior hippocampus but not in the middle or posterior hippocampus.
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FIG. 3.
Pattern of spatial and nonspatial delay activity across the 5-s delay period for anterior, middle, and posterior hippocampal delay neurons. The dotted line represents the baseline (ITI) activity level. Only data from inhibitory delay neurons are shown.
DISCUSSION
Abstract
Introduction
Methods
Results
Discussion
References
; Moser et al. 1993
) suggesting that the dorsal hippocampus (equivalent to the primate posterior hippocampus) is also more involved with processing spatial information than the ventral hippocampus (equivalent to the primate anterior hippocampus).
; Halgren 1991
; Sharp et al. 1995
) and that the hippocampus may be important for learning about directing movements to positions in space (Gaffan 1985
). To the extent that scalloping delay activity reflects a neural code of a response, our findings suggest that the anterior hippocampus may play a greater role in the motor aspects of spatial behavior than the posterior hippocampus. The fact that scalloping delay activity has been seen in the frontal cortex of monkeys (Fuster 1993
; Miller et al. 1996
) [a region strongly implicated in response planning and motor control (Boussaoud et al. 1996
; Petrides 1994
)] and that the anterior hippocampus has stronger projections with frontal cortex than the posterior hippocampus (Barbas and Blatt 1995
; Carmichael and Price 1995
) further supports this view.
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ACKNOWLEDGEMENTS |
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We thank Dr. Harlene Hayne for statistical assistance.
This research was supported by a University of Otago (Division of Sciences) sabbatical grant to M. Colombo, a Uehara Memorial Foundation grant to K. Nakamura, and National Eye Institute Grant EY-11347 to C. G. Gross.
Present addresses: T. Fernandez, Child Psychiatry Branch, National Institute of Mental Health, Bldg. 10, Rm. 3N202, Bethesda, MD 20892; K. Nakamura, Dept. of Behavioral and Brain Sciences, Primate Research Institute, Kyoto University, Kanrin, Inuyama, Aichi 484, Japan.
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FOOTNOTES |
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Address for reprint requests: M. Colombo, Dept. of Psychology, University of Otago, Dunedin, New Zealand.
Received 2 March 1998; accepted in final form 7 May 1998.
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REFERENCES |
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