As exampling the starfish to the octopi is of interest from sea to land, beaches to mountains and the intricate application and prowess of Man. These simple notes begin to etch the 'Missing Link' that Charles Darwin spoke of in his introduction to comprehend the evolution of what may have never referred to in their acknowledgement of his work but that I define as I was only born in 1965 and the City of San Francisco restricted a tad bit my growth in these subjects due to the overwhelming 1960s hell of religion and illicit drug use in my country the United States of America. As that era forced to much down the throats of city kids I relied upon The Cops (relate to a Catholic 'Father'. I.E. Priests) as my mentors and replaced all that religion with moral lessons taught by the de Young and Steinhart Aquarium (California Academy of Sciences) in Golden Gate Park with The Cops as my real moral compass.
That being said I again say that my life was restricted due to the religious practices of Christians, Mormons, Baptists, Protestants, Islam (Muslims), Catholics, Hippies (Hippie - Wikipedia), Women's Lib. (Women's liberation movement - Wikipedia), Moonies and so much more that I halted my interest and kept private by comprehension of all things only sharing with my mother Melba M. Meakin whom is now gone; the date of her succumb to death itself was January 11th, 2017 yet the adventure of our life began with:
The following video provided kindly by Youtube will give provisions to what my mother and I had battled from not only the City of San Francisco itself but will include the culmination of our country the United States of America and it's chaos as it chose the City of San Francisco to expose the "Human Being" and it is the chaotic Streets of San Francisco that she and I had to travel to just go from A to B, traveling each day from the Richmond District to downtown. This is to only introduce the average reader to the challenges of such times (the iconic 1960s, The Haight/Ashbury, etc.) and to allowance the average reader to that silence that had become our path in regards to the evolution of plant to man, dust to dust, ashes to ashes and so on.
The humpback whale to the mollusk as evolution's landing to understand that the mollusk is a Muscle and quite possibly the hippocampus of the human brain!! This video from Planet Earth Blue Planet II with David Attenborough thoroughly shows the evolution. As the hippocampus is represented far deeper than only the mullusk, this video provided by Youtube shows the magnificence of by design. From sea to land Man has developed, it is the ear of Planet Earth II that has filled in only the pictures of dreams for me. I present to you the dream in reality.
Hippocampus
Jump to navigation
Jump to search
The hippocampus (named after its resemblance to the seahorse, from the Greek ἱππόκαμπος, "seahorse" from ἵππος hippos, "horse" and κάμπος kampos, "sea monster") is a major component of the brains of humans and other vertebrates. Humans and other mammals have two hippocampi, one in each side of the brain. The hippocampus belongs to the limbic system and plays important roles in the consolidation of information from short-term memory to long-term memory, and in spatial memory that enables navigation. The hippocampus is located under the cerebral cortex (allocortical)[1][2][3] and in primates in the medial temporal lobe. It contains two main interlocking parts: the hippocampus proper (also called Ammon's horn)[4] and the dentate gyrus.
In Alzheimer's disease (and other forms of dementia), the hippocampus is one of the first regions of the brain to suffer damage; short-term memory loss and disorientation are included among the early symptoms. Damage to the hippocampus can also result from oxygen starvation (hypoxia), encephalitis, or medial temporal lobe epilepsy. People with extensive, bilateral hippocampal damage may experience anterograde amnesia (the inability to form and retain new memories).
In rodents as model organisms, the hippocampus has been studied extensively as part of a brain system responsible for spatial memory and navigation. Many neurons in the rat and mouse hippocampus respond as place cells: that is, they fire bursts of action potentials when the animal passes through a specific part of its environment. Hippocampal place cells interact extensively with head direction cells, whose activity acts as an inertial compass, and conjecturally with grid cells in the neighboring entorhinal cortex.
Since different neuronal cell types are neatly organized into layers in the hippocampus, it has frequently been used as a model system for studying neurophysiology. The form of neural plasticity known as long-term potentiation (LTP) was initially discovered to occur in the hippocampus and has often been studied in this structure. LTP is widely believed to be one of the main neural mechanisms by which memories are stored in the brain.
Hippocampus | |
---|---|
The hippocampus is located in the medial temporal lobe of the brain.
In this lateral view of the human brain, the frontal lobe is at the
left, the occipital lobe at the right, and the temporal and parietal
lobes have largely been removed to reveal the hippocampus underneath.
| |
Hippocampus (lowest pink bulb)
as part of the limbic system | |
Details | |
Part of | Temporal lobe |
Identifiers | |
Latin | Hippocampus |
NeuroLex ID | birnlex_721 |
TA | A14.1.09.321 |
FMA | 275020 |
Anatomical terms of neuroanatomy |
In Alzheimer's disease (and other forms of dementia), the hippocampus is one of the first regions of the brain to suffer damage; short-term memory loss and disorientation are included among the early symptoms. Damage to the hippocampus can also result from oxygen starvation (hypoxia), encephalitis, or medial temporal lobe epilepsy. People with extensive, bilateral hippocampal damage may experience anterograde amnesia (the inability to form and retain new memories).
In rodents as model organisms, the hippocampus has been studied extensively as part of a brain system responsible for spatial memory and navigation. Many neurons in the rat and mouse hippocampus respond as place cells: that is, they fire bursts of action potentials when the animal passes through a specific part of its environment. Hippocampal place cells interact extensively with head direction cells, whose activity acts as an inertial compass, and conjecturally with grid cells in the neighboring entorhinal cortex.
Since different neuronal cell types are neatly organized into layers in the hippocampus, it has frequently been used as a model system for studying neurophysiology. The form of neural plasticity known as long-term potentiation (LTP) was initially discovered to occur in the hippocampus and has often been studied in this structure. LTP is widely believed to be one of the main neural mechanisms by which memories are stored in the brain.
Contents
Name
The term limbic system was introduced in 1952 by Paul MacLean[11] to describe the set of structures that line the edge of the cortex (Latin limbus meaning border): These include the hippocampus, cingulate cortex, olfactory cortex, and amygdala. Paul MacLean later suggested that the limbic structures comprise the neural basis of emotion. The hippocampus is anatomically connected to parts of the brain that are involved with emotional behavior—the septum, the hypothalamic mammillary body, and the anterior nuclear complex in the thalamus, and is generally accepted to be part of the limbic system.[12]
Anatomy
The term hippocampal formation is used to refer to the hippocampus proper and its related parts. However, there is no consensus as to what parts are included. Sometimes the hippocampus is said to include the dentate gyrus and the subiculum. Some references include the dentate gyrus and the subiculum in the hippocampal formation,[1] and others also include the presubiculum, parasubiculum, and entorhinal cortex.[2] The neural layout and pathways within the hippocampal formation are very similar in all mammals.[3]
The hippocampus, including the dentate gyrus, has the shape of a curved tube, which has been compared to a seahorse, and a ram's horn (Cornu Ammonis). Its abbreviation CA is used in naming the hippocampal subfields CA1, CA2, CA3, and CA4.[16] It can be distinguished as an area where the cortex narrows into a single layer of densely packed pyramidal neurons, which curl into a tight U shape. One edge of the "U," – CA4, is embedded into the backward-facing, flexed dentate gyrus. The hippocampus is described as having an anterior and posterior part (in primates) or a ventral and dorsal part in other animals. Both parts are of similar composition but belong to different neural circuits.[18] In the rat, the two hippocampi resemble a pair of bananas, joined at the stems by the commissure of fornix (also called the hippocampal commissure). In primates, the part of the hippocampus at the bottom, near the base of the temporal lobe, is much broader than the part at the top. This means that in cross-section the hippocampus can show a number of different shapes, depending on the angle and location of the cut.
In a cross-section of the hippocampus, including the dentate gyrus, several layers will be shown. The dentate gyrus has three layers of cells (or four if the hilus is included). The layers are from the outer in - the molecular layer, the inner molecular layer, the granular layer, and the hilus. The CA3 in the hippocampus proper has the following cell layers known as strata: lacunosum-moleculare, radiatum, lucidum, pyramidal, and oriens. CA2 and CA1 also have four each of these layers and not the lucidum stratum.
The input to the hippocampus (from varying cortical and subcortical structures) comes from the entorhinal cortex via the perforant path. The entorhinal cortex (EC) is strongly and reciprocally connected with many cortical and subcortical structures as well as with the brainstem. Different thalamic nuclei, (from the anterior and midline groups), the medial septal nucleus, the supramamillary nucleus of the hypothalamus, and the raphe nuclei and locus coeruleus of the brainstem all send axons to the EC, so that it serves as the interface between the neocortex and the other connections, and the hippocampus.
The EC, is located in the parahippocampal gyrus,[2] a cortical region adjacent to the hippocampus.[19] This gyrus conceals the hippocampus. The parahippocampal gyrus also includes the perirhinal cortex which plays an important role in the visual recognition of complex objects. There is also substantial evidence that it makes a contribution to memory, which can be distinguished from the contribution of the hippocampus. It is apparent that complete amnesia occurs only when both the hippocampus and the parahippocampus are damaged.[19]
Circuitry
Basket cells in CA3 receive excitatory input from the pyramidal cells and then give an inhibitory feedback to the pyramidal cells. This recurrent inhibition is a simple feedback circuit that can dampen excitatory responses in the hippocampus. The pyramidal cells gives a recurrent excitation which is an important mechanism found in some memory processing microcircuits.[21]
Several other connections play important roles in hippocampal function.[16] Beyond the output to the EC, additional output pathways go to other cortical areas including the prefrontal cortex. A major output goes via the fornix to the lateral septal area and to the mammillary body of the hypothalamus (which the fornix interconnects with the hippocampus).[15] The hippocampus receives modulatory input from the serotonin, norepinephrine, and dopamine systems, and from the nucleus reuniens of the thalamus to field CA1. A very important projection comes from the medial septal nucleus, which sends cholinergic, and gamma amino butyric acid (GABA) stimulating fibers (GABAergic fibers) to all parts of the hippocampus. The inputs from the medial septal nucleus play a key role in controlling the physiological state of the hippocampus; destruction of this nucleus abolishes the hippocampal theta rhythm and severely impairs certain types of memory.[22]
Hippocampal regions
The intermediate hippocampus has overlapping characteristics with both the ventral and dorsal hippocampus.[23] Using anterograde tracing methods, Cenquizca and Swanson (2007) located the moderate projections to two primary olfactory cortical areas and prelimbic areas of the medial prefrontal cortex. This region has the smallest number of place cells. The ventral hippocampus functions in fear conditioning and affective processes.[26] Anagnostaras et al. (2002) showed that alterations to the ventral hippocampus reduced the amount of information sent to the amygdala by the dorsal and ventral hippocampus, consequently altering fear conditioning in rats.[27] Historically, the earliest widely held hypothesis was that the hippocampus is involved in olfaction.[28] This idea was cast into doubt by a series of anatomical studies that did not find any direct projections to the hippocampus from the olfactory bulb.[29] However, later work did confirm that the olfactory bulb does project into the ventral part of the lateral entorhinal cortex, and field CA1 in the ventral hippocampus sends axons to the main olfactory bulb,[30] the anterior olfactory nucleus, and to the primary olfactory cortex. There continues to be some interest in hippocampal olfactory responses, in particular, the role of the hippocampus in memory for odors, but few specialists today believe that olfaction is its primary function.[31][32]
Function
Theories of hippocampal functions
Over the years, three main ideas of hippocampal function have dominated the literature: response inhibition, episodic memory, and spatial cognition. The behavioral inhibition theory (caricatured by John O'Keefe and Lynn Nadel as "slam on the brakes!")[33] was very popular up to the 1960s. It derived much of its justification from two observations: first, that animals with hippocampal damage tend to be hyperactive; second, that animals with hippocampal damage often have difficulty learning to inhibit responses that they have previously been taught, especially if the response requires remaining quiet as in a passive avoidance test. Jeffrey Gray developed this line of thought into a full-fledged theory of the role of the hippocampus in anxiety.[34] The inhibition theory is currently the least popular of the three.[35]The second major line of thought relates the hippocampus to memory. Although it had historical precursors, this idea derived its main impetus from a famous report by William Beecher Scoville and Brenda Milner[36] describing the results of surgical destruction of the hippocampi (in an attempt to relieve epileptic seizures), in Henry Molaison,[37] known until his death in 2008 as "Patient H.M." The unexpected outcome of the surgery was severe anterograde and partial retrograde amnesia; Molaison was unable to form new episodic memories after his surgery and could not remember any events that occurred just before his surgery, but he did retain memories of events that occurred many years earlier extending back into his childhood. This case attracted such widespread professional interest that Molaison became the most intensively studied subject in medical history.[38] In the ensuing years, other patients with similar levels of hippocampal damage and amnesia (caused by accident or disease) have also been studied, and thousands of experiments have studied the physiology of activity-driven changes in synaptic connections in the hippocampus. There is now universal agreement that the hippocampi play some sort of important role in memory; however, the precise nature of this role remains widely debated.[39][40]
The third important theory of hippocampal function relates the hippocampus to space. The spatial theory was originally championed by O'Keefe and Nadel, who were influenced by E.C. Tolman's theories about "cognitive maps" in humans and animals. O'Keefe and his student Dostrovsky in 1971 discovered neurons in the rat hippocampus that appeared to them to show activity related to the rat's location within its environment.[41] Despite skepticism from other investigators, O'Keefe and his co-workers, especially Lynn Nadel, continued to investigate this question, in a line of work that eventually led to their very influential 1978 book The Hippocampus as a Cognitive Map.[42] There is now almost universal agreement that hippocampal function plays an important role in spatial coding, but the details are widely debated.[43]
Later research has focused on trying to bridge the disconnect between the two main views of hippocampal function as being split between memory and spatial cognition. In some studies, these areas have been expanded to the point of near convergence. In an attempt to reconcile the two disparate views it is suggested that a broader view of the hippocampal function is taken and seen to have a role that encompasses both the organisation of experience (mental mapping), (as per Tolman's original concept in 1948) and the directional behaviour seen as being involved in all areas of cognition. So that the function of the hippocampus can be viewed as a broader system that incorporates both the memory and the spatial perspectives in its role that involves the use of a wide scope of cognitive maps.[44] This relates to the purposive behaviorism born of Tolman's original goal of identifying the complex cognitive mechanisms and purposes that guided behaviour.[45]
It has also been proposed that the spiking activity of hippocampal neurons is associated spatially, and it was suggested that the mechanisms of memory and planning both evolved from mechanisms of navigation and that their neuronal algorithms were basically the same.[46]
Many studies have made use of neuroimaging techniques such as functional magnetic resonance imaging (fMRI) and a functional role in approach-avoidance conflict has been noted. The anterior hippocampus is seen to be involved in decision-making under approach-avoidance conflict processing. It is suggested that the memory, spatial cognition, and conflict processing functions may be seen as working together and not mutually exclusive.[47]
Role in memory
Psychologists and neuroscientists generally agree that the hippocampus plays an important role in the formation of new memories about experienced events (episodic or autobiographical memory).[40][48] Part of this function is hippocampal involvement in the detection of new events, places and stimuli.[49] Some researchers regard the hippocampus as part of a larger medial temporal lobe memory system responsible for general declarative memory (memories that can be explicitly verbalized—these would include, for example, memory for facts in addition to episodic memory).[39] The hippocampus also encodes emotional context from the amygdala. This is partly why returning to a location where an emotional event occurred may evoke that emotion. There is a deep emotional connection between episodic memories and places.[50]Due to bilateral symmetry the brain has a hippocampus in each cerebral hemisphere. If damage to the hippocampus occurs in only one hemisphere, leaving the structure intact in the other hemisphere, the brain can retain near-normal memory functioning.[51] Severe damage to the hippocampi in both hemispheres results in profound difficulties in forming new memories (anterograde amnesia) and often also affects memories formed before the damage occurred (retrograde amnesia). Although the retrograde effect normally extends many years back before the brain damage, in some cases older memories remain. This retention of older memories leads to the idea that consolidation over time involves the transfer of memories out of the hippocampus to other parts of the brain.[52] Experiments using intrahippocampal transplantation of hippocampal cells in primates with neurotoxic lesions of the hippocampus have shown that the hippocampus is required for the formation and recall, but not the storage, of memories.[53]
Damage to the hippocampus does not affect some types of memory, such as the ability to learn new skills (playing a musical instrument or solving certain types of puzzles, for example). This fact suggests that such abilities depend on different types of memory (procedural memory) and different brain regions. Furthermore, amnesic patients frequently show "implicit" memory for experiences even in the absence of conscious knowledge. For example, patients asked to guess which of two faces they have seen most recently may give the correct answer most of the time in spite of stating that they have never seen either of the faces before. Some researchers distinguish between conscious recollection, which depends on the hippocampus, and familiarity, which depends on portions of the medial temporal lobe.[54]
In humans, cells with location-specific firing patterns have been reported during a study of patients with drug-resistant epilepsy. They were undergoing an invasive procedure to localize the source of their seizures, with a view to surgical resection. The patients had diagnostic electrodes implanted in their hippocampus and then used a computer to move around in a virtual reality town.[59] Similar brain imaging studies in navigation have shown the hippocampus to be active.[60] A study was carried out on taxi drivers. London’s black cab drivers need to learn the locations of a large number of places and the fastest routes between them in order to pass a strict test known as The Knowledge in order to gain a license to operate. A study showed that the posterior part of the hippocampus is larger in these drivers than in the general public, and that a positive correlation exists between the length of time served as a driver and the increase in the volume of this part. It was also found the total volume of the hippocampus was unchanged, as the increase seen in the posterior part was made at the expense of the anterior part, which showed a relative decrease in size. There have been no reported adverse effects from this disparity in hippocampal proportions.[61] Another study showed opposite findings in blind individuals. The anterior part of the right hippocampus was larger and the posterior part was smaller, comparing with sighted individuals.[62]
There are several navigational cells in the brain that are either in the hippocampus itself or are strongly connected to it, such as the speed cells present in the medial entorhinal cortex. Together these cells form a network that serves as spatial memory. The first of such cells discovered in the 1970s were the place cells, which led to the idea of the hippocampus acting to give a neural representation of the environment in a cognitive map.[63] When the hippocampus is dysfunctional, orientation is affected; people may have difficulty in remembering how they arrived at a location and how to proceed further. Getting lost is a common symptom of amnesia.[64] Studies with animals have shown that an intact hippocampus is required for initial learning and long-term retention of some spatial memory tasks, in particular ones that require finding the way to a hidden goal.[65][66][67][68] Other cells have been discovered since the finding of the place cells in the rodent brain that are either in the hippocampus or the entorhinal cortex. These have been assigned as head direction cells, grid cells and boundary cells.[43][69] Speed cells are thought to provide input to the hippocampal grid cells.
Role in approach-avoidance conflict processing
Approach-avoidance conflict happens when a situation is presented that can either be rewarding or punishing, and the ensuing decision-making has been associated with anxiety.[70] fMRI findings from studies in approach-avoidance decision-making found evidence for a functional role that is not explained by either long-term memory or spatial cognition. Overall findings showed that the anterior hippocampus is sensitive to conflict, and that it may be part of a larger cortical and subcortical network seen to be important in decision making in uncertain conditions.[70]A review makes reference to a number of studies that show the involvement of the hippocampus in conflict tasks. The authors suggest that a challenge is to understand how conflict processing relates to the functions of spatial navigation and memory and how all of these functions need not be mutually exclusive.[47]
Physiology
The theta mode appears during states of active, alert behavior (especially locomotion), and also during REM (dreaming) sleep.[72] In the theta mode, the EEG is dominated by large regular waves with a frequency range of 6 to 9 Hz, and the main groups of hippocampal neurons (pyramidal cells and granule cells) show sparse population activity, which means that in any short time interval, the great majority of cells are silent, while the small remaining fraction fire at relatively high rates, up to 50 spikes in one second for the most active of them. An active cell typically stays active for half a second to a few seconds. As the rat behaves, the active cells fall silent and new cells become active, but the overall percentage of active cells remains more or less constant. In many situations, cell activity is determined largely by the spatial location of the animal, but other behavioral variables also clearly influence it.
The LIA mode appears during slow-wave (non-dreaming) sleep, and also during states of waking immobility such as resting or eating.[72] In the LIA mode, the EEG is dominated by sharp waves that are randomly timed large deflections of the EEG signal lasting for 25–50 milliseconds. Sharp waves are frequently generated in sets, with sets containing up to 5 or more individual sharp waves and lasting up to 500 ms. The spiking activity of neurons within the hippocampus is highly correlated with sharp wave activity. Most neurons decrease their firing rate between sharp waves; however, during a sharp wave, there is a dramatic increase in firing rate in up to 10% of the hippocampal population
These two hippocampal activity modes can be seen in primates as well as rats, with the exception that it has been difficult to see robust theta rhythmicity in the primate hippocampus. There are, however, qualitatively similar sharp waves and similar state-dependent changes in neural population activity.[73]
Theta rhythm
Theta rhythmicity is very obvious in rabbits and rodents and also clearly present in cats and dogs. Whether theta can be seen in primates is not yet clear.[77] In rats (the animals that have been the most extensively studied), theta is seen mainly in two conditions: first, when an animal is walking or in some other way actively interacting with its surroundings; second, during REM sleep.[78] The function of theta has not yet been convincingly explained although numerous theories have been proposed.[71] The most popular hypothesis has been to relate it to learning and memory. An example would be the phase with which theta rhythms, at the time of stimulation of a neuron, shape the effect of that stimulation upon its synapses. What is meant here is that theta rhythms may affect those aspects of learning and memory that are dependent upon synaptic plasticity.[79] It is well established that lesions of the medial septum—the central node of the theta system—cause severe disruptions of memory. However, the medial septum is more than just the controller of theta; it is also the main source of cholinergic projections to the hippocampus.[16] It has not been established that septal lesions exert their effects specifically by eliminating the theta rhythm.[80]
Sharp waves
During sleep or during resting, when an animal is not engaged with its surroundings, the hippocampal EEG shows a pattern of irregular slow waves, somewhat larger in amplitude than theta waves. This pattern is occasionally interrupted by large surges called sharp waves.[81] These events are associated with bursts of spike activity lasting 50 to 100 milliseconds in pyramidal cells of CA3 and CA1. They are also associated with short-lived high-frequency EEG oscillations called "ripples", with frequencies in the range 150 to 200 Hz in rats, and together they are known as sharp waves and ripples. Sharp waves are most frequent during sleep when they occur at an average rate of around 1 per second (in rats) but in a very irregular temporal pattern. Sharp waves are less frequent during inactive waking states and are usually smaller. Sharp waves have also been observed in humans and monkeys. In macaques, sharp waves are robust but do not occur as frequently as in rats.[73]One of the most interesting aspects of sharp waves is that they appear to be associated with memory. Wilson and McNaughton 1994,[82] and numerous later studies, reported that when hippocampal place cells have overlapping spatial firing fields (and therefore often fire in near-simultaneity), they tend to show correlated activity during sleep following the behavioral session. This enhancement of correlation, commonly known as reactivation, has been found to occur mainly during sharp waves.[83] It has been proposed that sharp waves are, in fact, reactivations of neural activity patterns that were memorized during behavior, driven by strengthening of synaptic connections within the hippocampus.[84] This idea forms a key component of the "two-stage memory" theory, advocated by Buzsáki and others, which proposes that memories are stored within the hippocampus during behavior and then later transferred to the neocortex during sleep. Sharp waves in Hebbian theory are seen as persistently repeated stimulations by presynaptic cells, of postsynaptic cells that are suggested to drive synaptic changes in the cortical targets of hippocampal output pathways.[85] Suppression of sharp waves and ripples in sleep or during immobility can interfere with memories expressed at the level of the behavior,[86][87] nonetheless, the newly formed CA1 place cell code can re-emerge even after a sleep with abolished sharp waves and ripples, in spatially non-demanding tasks.[88]
Long-term potentiation
Since at least the time of Ramon y Cajal (1852-1934), psychologists have speculated that the brain stores memory by altering the strength of connections between neurons that are simultaneously active.[89] This idea was formalized by Donald Hebb in 1949,[90] but for many years remained unexplained. In 1973, Tim Bliss and Terje Lømo described a phenomenon in the rabbit hippocampus that appeared to meet Hebb's specifications: a change in synaptic responsiveness induced by brief strong activation and lasting for hours or days or longer.[91] This phenomenon was soon referred to as long-term potentiation (LTP). As a candidate mechanism for long-term memory, LTP has since been studied intensively, and a great deal has been learned about it. However, the complexity and variety of the intracellular signalling cascades that can trigger LTP is acknowledged as preventing a more complete understanding.[92]The hippocampus is a particularly favorable site for studying LTP because of its densely packed and sharply defined layers of neurons, but similar types of activity-dependent synaptic change have also been observed in many other brain areas.[93] The best-studied form of LTP has been seen in CA1 of the hippocampus and occurs at synapses that terminate on dendritic spines and use the neurotransmitter glutamate.[92] The synaptic changes depend on a special type of glutamate receptor, the N-methyl-D-aspartate (NMDA) receptor, a cell surface receptor which has the special property of allowing calcium to enter the postsynaptic spine only when presynaptic activation and postsynaptic depolarization occur at the same time.[94] Drugs that interfere with NMDA receptors block LTP and have major effects on some types of memory, especially spatial memory. Genetically modified mice that are modified to disable the LTP mechanism, also generally show severe memory deficits.[94]
Pathology
Aging
Age-related conditions such as Alzheimer's disease and other forms of dementia (for which hippocampal disruption is one of the earliest signs[95]) have a severe impact on many types of cognition, but even normal aging is associated with a gradual decline in some types of memory, including episodic memory and working memory (or short-term memory). Because the hippocampus is thought to play a central role in memory, there has been considerable interest in the possibility that age-related declines could be caused by hippocampal deterioration.[96] Some early studies reported substantial loss of neurons in the hippocampus of elderly people, but later studies using more precise techniques found only minimal differences.[96] Similarly, some MRI studies have reported shrinkage of the hippocampus in elderly people, but other studies have failed to reproduce this finding. There is, however, a reliable relationship between the size of the hippocampus and memory performance; so that where there is age-related shrinkage, memory performance will be impaired.[97] There are also reports that memory tasks tend to produce less hippocampal activation in the elderly than in the young.[97] Furthermore, a randomized control trial published in 2011 found that aerobic exercise could increase the size of the hippocampus in adults aged 55 to 80 and also improve spatial memory.[98]Effects of cortisol
The hippocampus contains high levels of glucocorticoid receptors, which make it more vulnerable to long-term stress than most other brain areas.[99] There is evidence that humans having experienced severe, long-lasting traumatic stress show atrophy of the hippocampus more than of other parts of the brain.[100] These effects show up in post-traumatic stress disorder,[101] and they may contribute to the hippocampal atrophy reported in schizophrenia[102] and severe depression.[103] A recent study has also revealed atrophy as a result of depression, but this can be stopped with anti-depressants even if they are not effective in relieving other symptoms.[104]Chronic stress resulting in elevated levels of glucocorticoids, notably of cortisol, is seen to be a cause of neuronal atrophy in the hippocampus.This atrophy results in a smaller hippocampal volume which is also seen in Cushing’s syndrome. The higher levels of cortisol in Cushing’s syndrome is usually the result of medications taken for other conditions.[105][106] Neuronal loss also occurs as a result of impaired neurogenesis. Another factor that contributes to a smaller hippocampal volume is that of dendritic retraction where dendrites are shortened in length and reduced in number, in response to increased glucocorticoids. This dendritic retraction is reversible.[106] After treatment with medication to reduce cortisol in Cushing’s syndrome, the hippocampal volume is seen to be restored by as much as 10%.[105] This change is seen to be due to the reforming of the dendrites.[106] This dendritic restoration can also happen when stress is removed. There is, however, evidence derived mainly from studies using rats that stress occurring shortly after birth can affect hippocampal function in ways that persist throughout life.[107]
Sex-specific responses to stress have also been demonstrated in the rat to have an effect on the hippocampus. Chronic stress in the male rat showed dendritic retraction and cell loss in the CA3 region but this was not shown in the female. This was thought to be due to neuroprotective ovarian hormones.[108][109] In rats, DNA damage increases in the hippocampus under conditions of stress.[110]
Epilepsy
Seizures in temporal lobe epilepsy can affect the normal development of new neurons and can cause tissue damage. Hippocampal sclerosis is the most common type of such tissue damage.[113] It is not yet clear, however, whether the epilepsy is usually caused by hippocampal abnormalities or whether the hippocampus is damaged by cumulative effects of seizures.[114] However, in experimental settings where repetitive seizures are artificially induced in animals, hippocampal damage is a frequent result. This may be a consequence of the concentration of excitable glutamate receptors in the hippocampus. Hyperexcitability can lead to cytotoxicity and cell death.[106] It may also have something to do with the hippocampus being a site where new neurons continue to be created throughout life,[115] and to abnormalities in this process.[106]
Schizophrenia
The causes of schizophrenia are not well understood, but numerous abnormalities of brain structure have been reported. The most thoroughly investigated alterations involve the cerebral cortex, but effects on the hippocampus have also been described. Many reports have found reductions in the size of the hippocampus in schizophrenic subjects.[116][117] The left hippocampus seems to be affected more than the right.[116] The changes noted have largely been accepted to be the result of abnormal development. It is unclear whether hippocampal alterations play any role in causing the psychotic symptoms that are the most important feature of schizophrenia. It has been suggested that on the basis of experimental work using animals, hippocampal dysfunction might produce an alteration of dopamine release in the basal ganglia, thereby indirectly affecting the integration of information in the prefrontal cortex.[118] It has also been suggested that hippocampal dysfunction might account for the disturbances in long-term memory frequently observed.[119]MRI studies have found a smaller brain volume and larger ventricles in people with schizophrenia–however researchers do not know if the shrinkage is from the schizophrenia or from the medication.[120][121] The hippocampus and thalamus have been shown to be reduced in volume; and the volume of the globus pallidus is increased. Cortical patterns are altered, and a reduction in the volume and thickness of the cortex particularly in the frontal and temporal lobes has been noted. It has further been proposed that many of the changes seen are present at the start of the disorder which gives weight to the theory that there is abnormal neurodevelopment.[122]
The hippocampus has been seen as central to the pathology of schizophrenia, both in the neural and physiological effects.[116] It has been generally accepted that there is an abnormal synaptic connectivity underlying schizophrenia. Several lines of evidence implicate changes in the synaptic organization and connectivity, in and from the hippocampus[116] Many studies have found dysfunction in the synaptic circuitry within the hippocampus and its activity on the prefrontal cortex. The glutamatergic pathways have been seen to be largely affected. The subfield CA1 is seen to be the least involved of the other subfields,[116][123] and CA4 and the subiculum have been reported elsewhere as being the most implicated areas.[123] The review concluded that the pathology could be due to genetics, faulty neurodevelopment or abnormal neural plasticity. It was further concluded that schizophrenia is not due to any known neurodegenerative disorder.[116] Oxidative DNA damage is substantially increased in the hippocampus of elderly patients with chronic schizophrenia.[124]
Transient global amnesia
Transient global amnesia is a dramatic, sudden, temporary, near-total loss of short-term memory. Various causes have been hypothesized including ischemia, epilepsy, migraine[125] and disturbance of cerebral venous blood flow,[126] leading to ischemia of structures such as the hippocampus that are involved in memory.[127]There has been no scientific proof of any cause. However, diffusion weighted MRI studies taken from 12–24 hours following an episode has shown there to be small dot-like lesions in the hippocampus. These findings have suggested a possible implication of CA1 neurons made vulnerable by metabolic stress.[125]
PTSD
Some studies shows correlation of reduced hippocampus volume and posttraumatic stress disorder (PTSD).[128][129][130] A study of Vietnam War combat veterans with PTSD showed a 20% reduction in the volume of their hippocampus compared with veterans having suffered no such symptoms.[131] This finding was not replicated in chronic PTSD patients traumatized at an air show plane crash in 1988 (Ramstein, Germany).[132] A 2016 study strengthened theory that a smaller hippocampus increases the risk for post-traumatic stress disorder, and a larger hippocampus increases the likelihood of efficacious treatment.[133]Other animals
There is also a general relationship between the size of the hippocampus and spatial memory. When comparisons are made between similar species, those that have a greater capacity for spatial memory tend to have larger hippocampal volumes.[136] This relationship also extends to sex differences; in species where males and females show strong differences in spatial memory ability they also tend to show corresponding differences in hippocampal volume.[137]
Non-mammalian species do not have a brain structure that looks like the mammalian hippocampus, but they have one that is considered homologous to it. The hippocampus, as pointed out above, is in essence part of the allocortex. Only mammals have a fully developed cortex, but the structure it evolved from, called the pallium, is present in all vertebrates, even the most primitive ones such as the lamprey or hagfish.[138] The pallium is usually divided into three zones: medial, lateral and dorsal. The medial pallium forms the precursor of the hippocampus. It does not resemble the hippocampus visually because the layers are not warped into an S shape or enfolded by the dentate gyrus, but the homology is indicated by strong chemical and functional affinities. There is now evidence that these hippocampal-like structures are involved in spatial cognition in birds, reptiles, and fish.[139]
In birds, the correspondence is sufficiently well established that most anatomists refer to the medial pallial zone as the "avian hippocampus".[140] Numerous species of birds have strong spatial skills, in particular those that cache food. There is evidence that food-caching birds have a larger hippocampus than other types of birds and that damage to the hippocampus causes impairments in spatial memory.[141]
The story for fish is more complex. In teleost fish (which make up the great majority of existing species), the forebrain is distorted in comparison to other types of vertebrates: Most neuroanatomists believe that the teleost forebrain is in essence everted, like a sock turned inside-out, so that structures that lie in the interior, next to the ventricles, for most vertebrates, are found on the outside in teleost fish, and vice versa.[142] One of the consequences of this is that the medial pallium ("hippocampal" zone) of a typical vertebrate is thought to correspond to the lateral pallium of a typical fish. Several types of fish (particularly goldfish) have been shown experimentally to have strong spatial memory abilities, even forming "cognitive maps" of the areas they inhabit.[136] There is evidence that damage to the lateral pallium impairs spatial memory.[143][144]
It is not yet known whether the medial pallium plays a similar role in even more primitive vertebrates, such as sharks and rays, or even lampreys and hagfish. Some types of insects, and molluscs such as the octopus, also have strong spatial learning and navigation abilities, but these appear to work differently from the mammalian spatial system, so there is as yet no good reason to think that they have a common evolutionary origin; nor is there sufficient similarity in brain structure to enable anything resembling a "hippocampus" to be identified in these species. Some have proposed, however, that the insect's mushroom bodies may have a function similar to that of the hippocampus.[145]
Additional images
- Morphology in four rodent species
- Main hippocampal regions in marmoset
- Neuronal loss shown in rat CA1 following ischemia
See also
Notes
The 2017 version of this article has passed academic peer review (here) and was published in WikiJournal of Medicine .
It can be cited as: Wright M, et al. (2017). "The Hippocampus". WikiJournal of Medicine. 4 (1): 3. doi:10.15347/wjm/2017.003. |
- References
References
- Aboitiz F, Morales D, Montiel J (Oct 2003). "The evolutionary origin of the mammalian isocortex: towards an integrated developmental and functional approach". The Behavioral and Brain Sciences. 26 (5): 535–52. doi:10.1017/S0140525X03000128. PMID 15179935.
- Amaral D, Lavenex P (2006). "Ch 3. Hippocampal Neuroanatomy". In Andersen P, Morris R, Amaral D, Bliss T, O'Keefe J. The Hippocampus Book. Oxford University Press. ISBN 978-0-19-510027-3.
- Anagnostaras SG, Gale GD, Fanselow MS (2002). "The hippocampus and Pavlovian fear conditioning: reply to Bast et al" (PDF). Hippocampus. 12 (4): 561–565. doi:10.1002/hipo.10071. PMID 12201641. Archived from the original (PDF) on 2005-02-16.
- Best PJ, White AM (1999). "Placing hippocampal single-unit studies in a historical context". Hippocampus. 9 (4): 346–51. doi:10.1002/(SICI)1098-1063(1999)9:4<346::AID-HIPO2>3.0.CO;2-3. PMID 10495017.
- Bliss TV, Lomo T (Jul 1973). "Long-lasting potentiation of synaptic transmission in the dentate area of the anaesthetized rabbit following stimulation of the perforant path". The Journal of Physiology. 232 (2): 331–56. doi:10.1113/jphysiol.1973.sp010273. PMC 1350458. PMID 4727084.
- Boyer P, Phillips JL, Rousseau FL, Ilivitsky S (Apr 2007). "Hippocampal abnormalities and memory deficits: new evidence of a strong pathophysiological link in schizophrenia". Brain Research Reviews. 54 (1): 92–112. doi:10.1016/j.brainresrev.2006.12.008. PMID 17306884.
- Broglio C, Gómez A, Durán E, Ocaña FM, Jiménez-Moya F, Rodríguez F, Salas C (Sep 2005). "Hallmarks of a common forebrain vertebrate plan: specialized pallial areas for spatial, temporal and emotional memory in actinopterygian fish". Brain Research Bulletin. 66 (4–6): 397–99. doi:10.1016/j.brainresbull.2005.03.021. PMID 16144602.
- Burke SN, Barnes CA (Jan 2006). "Neural plasticity in the ageing brain". Nature Reviews. Neuroscience. 7 (1): 30–40. doi:10.1038/nrn1809. PMID 16371948.
- Buzsáki G (Nov 1986). "Hippocampal sharp waves: their origin and significance". Brain Research. 398 (2): 242–52. doi:10.1016/0006-8993(86)91483-6. PMID 3026567.
- Buzsáki G (1989). "Two-stage model of memory trace formation: a role for "noisy" brain states". Neuroscience. 31 (3): 551–70. doi:10.1016/0306-4522(89)90423-5. PMID 2687720.
- Buzsáki G, Chen LS, Gage FH (1990). "Spatial organization of physiological activity in the hippocampal region: relevance to memory formation". Progress in Brain Research. 83: 257–68. doi:10.1016/S0079-6123(08)61255-8. ISBN 9780444811493. PMID 2203100.
- Buzsáki G (Jan 2002). "Theta oscillations in the hippocampus" (PDF). Neuron. 33 (3): 325–40. doi:10.1016/S0896-6273(02)00586-X. PMID 11832222. Archived from the original (PDF) on 2008-06-25.
- Ramón y Cajal S (1894). "The Croonian Lecture: La Fine Structure des Centres Nerveux". Proceedings of the Royal Society. 55 (331–335): 444–68. doi:10.1098/rspl.1894.0063.
- Campbell S, Macqueen G (Nov 2004). "The role of the hippocampus in the pathophysiology of major depression". Journal of Psychiatry & Neuroscience. 29 (6): 417–26. PMC 524959. PMID 15644983.
- Cantero JL, Atienza M, Stickgold R, Kahana MJ, Madsen JR, Kocsis B (Nov 2003). "Sleep-dependent theta oscillations in the human hippocampus and neocortex". The Journal of Neuroscience. 23 (34): 10897–903. PMID 14645485.
- Carey B (2008-12-04). "H. M., an Unforgettable Amnesiac, Dies at 82". The New York Times. Retrieved 2009-04-27.
- Chiu YC, Algase D, Whall A, Liang J, Liu HC, Lin KN, Wang PN (2004). "Getting lost: directed attention and executive functions in early Alzheimer's disease patients". Dementia and Geriatric Cognitive Disorders. 17 (3): 174–80. doi:10.1159/000076353. PMID 14739541.
- Chang BS, Lowenstein DH (Sep 2003). "Epilepsy". The New England Journal of Medicine. 349 (13): 1257–66. doi:10.1056/NEJMra022308. PMID 14507951.
- Cho RY, Gilbert A, Lewis DA (2005). "Ch 22. The neurobiology of schizophrenia". In Charney DS, Nestler EJ. Neurobiology of Mental Illness. Oxford University Press US. ISBN 978-0-19-518980-3.
- Cenquizca LA, Swanson LW (Nov 2007). "Spatial organization of direct hippocampal field CA1 axonal projections to the rest of the cerebral cortex". Brain Research Reviews. 56 (1): 1–26. doi:10.1016/j.brainresrev.2007.05.002. PMC 2171036. PMID 17559940.
- Clark RE, Broadbent NJ, Squire LR (2005). "Hippocampus and remote spatial memory in rats". Hippocampus. 15 (2): 260–72. doi:10.1002/hipo.20056. PMC 2754168. PMID 15523608.
- Colombo M, Broadbent N (Jun 2000). "Is the avian hippocampus a functional homologue of the mammalian hippocampus?". Neuroscience and Biobehavioral Reviews. 24 (4): 465–84. doi:10.1016/S0149-7634(00)00016-6. PMID 10817844.
- Cooke SF, Bliss TV (Jul 2006). "Plasticity in the human central nervous system". Brain. 129 (Pt 7): 1659–73. doi:10.1093/brain/awl082. PMID 16672292.
- de Olmos J, Hardy H, Heimer L (Sep 1978). "The afferent connections of the main and the accessory olfactory bulb formations in the rat: an experimental HRP-study". The Journal of Comparative Neurology. 181 (2): 213–244. doi:10.1002/cne.901810202. PMID 690266.
- Diana RA, Yonelinas AP, Ranganath C (Sep 2007). "Imaging recollection and familiarity in the medial temporal lobe: a three-component model". Trends in Cognitive Sciences. 11 (9): 379–86. doi:10.1016/j.tics.2007.08.001. PMID 17707683.
- Duvernoy HM (2005). "Introduction". The Human Hippocampus (3rd ed.). Berlin: Springer-Verlag. p. 1. ISBN 978-3-540-23191-2.
- Eichenbaum H, Otto TA, Wible CG, Piper JM (1991). "Ch 7. Building a model of the hippocampus in olfaction and memory". In Davis JL, Eichenbaum H. Olfaction. MIT Press. ISBN 978-0-262-04124-9.
- Eichenbaum H, Cohen NJ (1993). Memory, Amnesia, and the Hippocampal System. MIT Press.
- Eichenbaum H, Yonelinas AP, Ranganath C (2007). "The medial temporal lobe and recognition memory". Annual Review of Neuroscience. 30: 123–52. doi:10.1146/annurev.neuro.30.051606.094328. PMC 2064941. PMID 17417939.
- Ekstrom AD, Kahana MJ, Caplan JB, Fields TA, Isham EA, Newman EL, Fried I (Sep 2003). "Cellular networks underlying human spatial navigation" (PDF). Nature. 425 (6954): 184–88. Bibcode:2003Natur.425..184E. CiteSeerX 10.1.1.408.4443. doi:10.1038/nature01964. PMID 12968182.
- Erickson KI, et al. (Feb 2011). "Exercise training increases size of hippocampus and improves memory". Proceedings of the National Academy of Sciences of the United States of America. 108 (7): 3017–3022. Bibcode:2011PNAS..108.3017E. doi:10.1073/pnas.1015950108. PMC 3041121. PMID 21282661.
- Fanselow MS, Dong HW (Jan 2010). "Are the dorsal and ventral hippocampus functionally distinct structures?" (PDF). Neuron. 65 (1): 7–19. doi:10.1016/j.neuron.2009.11.031. PMC 2822727. PMID 20152109.
- Finger, S (2001). Origins of Neuroscience: A History of Explorations Into Brain Function. Oxford University Press US. ISBN 978-0-19-514694-3.
- Garcia-Segura LM (2009). Hormones and Brain Plasticity. Oxford University Press US. ISBN 978-0-19-532661-1.
- Woon FL, Sood S, Hedges DW (Oct 2010). "Hippocampal volume deficits associated with exposure to psychological trauma and posttraumatic stress disorder in adults: a meta-analysis". Progress in Neuro-Psychopharmacology & Biological Psychiatry. 34 (7): 1181–1188. doi:10.1016/j.pnpbp.2010.06.016. PMID 20600466.
- Gorwood P, Corruble E, Falissard B, Goodwin GM (Jun 2008). "Toxic effects of depression on brain function: impairment of delayed recall and the cumulative length of depressive disorder in a large sample of depressed outpatients". The American Journal of Psychiatry. 165 (6): 731–9. doi:10.1176/appi.ajp.2008.07040574. PMID 18381906.
- Goto Y, Grace AA (Nov 2008). "Limbic and cortical information processing in the nucleus accumbens". Trends in Neurosciences. 31 (11): 552–8. doi:10.1016/j.tins.2008.08.002. PMC 2884964. PMID 18786735.
- Gray JA, McNaughton N (2000). The Neuropsychology of Anxiety: An Enquiry into the Functions of the Septo-Hippocampal System. Oxford University Press.
- Gross CG (Oct 1993). "Hippocampus minor and man's place in nature: a case study in the social construction of neuroanatomy". Hippocampus. 3 (4): 403–416. doi:10.1002/hipo.450030403. PMID 8269033.
- Hampel H, Bürger K, Teipel SJ, Bokde AL, Zetterberg H, Blennow K (Jan 2008). "Core candidate neurochemical and imaging biomarkers of Alzheimer's disease". Alzheimer's & Dementia. 4 (1): 38–48. doi:10.1016/j.jalz.2007.08.006. PMID 18631949.
- Harrison PJ (Jun 2004). "The hippocampus in schizophrenia: a review of the neuropathological evidence and its pathophysiological implications". Psychopharmacology. 174 (1): 151–62. doi:10.1007/s00213-003-1761-y. PMID 15205886.
- Hebb DO (1949). Organization of Behavior: a Neuropsychological Theory. New York: John Wiley. ISBN 978-0-471-36727-7.
- Huerta PT, Lisman JE (Aug 1993). "Heightened synaptic plasticity of hippocampal CA1 neurons during a cholinergically induced rhythmic state". Nature. 364 (6439): 723–5. Bibcode:1993Natur.364..723H. doi:10.1038/364723a0. PMID 8355787.
- Jackson JC, Johnson A, Redish AD (Nov 2006). "Hippocampal sharp waves and reactivation during awake states depend on repeated sequential experience". The Journal of Neuroscience. 26 (48): 12415–26. doi:10.1523/JNEUROSCI.4118-06.2006. PMID 17135403.
- Jacobs LF, Gaulin SJ, Sherry DF, Hoffman GE (Aug 1990). "Evolution of spatial cognition: sex-specific patterns of spatial behavior predict hippocampal size". Proceedings of the National Academy of Sciences of the United States of America. 87 (16): 6349–52. Bibcode:1990PNAS...87.6349J. doi:10.1073/pnas.87.16.6349. PMC 54531. PMID 2201026.
- Jacobs LF (2003). "The evolution of the cognitive map". Brain, Behavior and Evolution. 62 (2): 128–39. doi:10.1159/000072443. PMID 12937351.
- Jung MW, Wiener SI, McNaughton BL (Dec 1994). "Comparison of spatial firing characteristics of units in dorsal and ventral hippocampus of the rat". The Journal of Neuroscience. 14 (12): 7347–7356. PMID 7996180.
- Kahana MJ, Seelig D, Madsen JR (Dec 2001). "Theta returns". Current Opinion in Neurobiology. 11 (6): 739–44. doi:10.1016/S0959-4388(01)00278-1. PMID 11741027.
- Kötter R, Stephan KE (1997). "Useless or helpful? The "limbic system" concept". Reviews in the Neurosciences. 8 (2): 139–45. doi:10.1515/REVNEURO.1997.8.2.139. PMID 9344183.
- Joëls M (Apr 2008). "Functional actions of corticosteroids in the hippocampus". European Journal of Pharmacology. 583 (2–3): 312–321. doi:10.1016/j.ejphar.2007.11.064. PMID 18275953.
- Kuruba R, Hattiangady B, Shetty AK (Jan 2009). "Hippocampal neurogenesis and neural stem cells in temporal lobe epilepsy". Epilepsy & Behavior. 14 Suppl 1: 65–73. doi:10.1016/j.yebeh.2008.08.020. PMC 2654382. PMID 18796338.
- Lubenov EV, Siapas AG (May 2009). "Hippocampal theta oscillations are travelling waves". Nature. 459 (7246): 534–9. Bibcode:2009Natur.459..534L. doi:10.1038/nature08010. PMID 19489117.
- Maguire EA, Burgess N, Donnett JG, Frackowiak RS, Frith CD, O'Keefe J (May 1998). "Knowing where and getting there: a human navigation network". Science. 280 (5365): 921–24. Bibcode:1998Sci...280..921M. CiteSeerX 10.1.1.23.4963. doi:10.1126/science.280.5365.921. PMID 9572740.
- Maguire EA, Gadian DG, Johnsrude IS, Good CD, Ashburner J, Frackowiak RS, Frith CD (Apr 2000). "Navigation-related structural change in the hippocampi of taxi drivers". Proceedings of the National Academy of Sciences of the United States of America. 97 (8): 4398–403. Bibcode:2000PNAS...97.4398M. doi:10.1073/pnas.070039597. PMC 18253. PMID 10716738.
- Malenka RC, Bear MF (Sep 2004). "LTP and LTD: an embarrassment of riches". Neuron. 44 (1): 5–21. doi:10.1016/j.neuron.2004.09.012. PMID 15450156.
- Matsumura N, Nishijo H, Tamura R, Eifuku S, Endo S, Ono T (Mar 1999). "Spatial- and task-dependent neuronal responses during real and virtual translocation in the monkey hippocampal formation". The Journal of Neuroscience. 19 (6): 2381–93. PMID 10066288.
- McNaughton BL, Battaglia FP, Jensen O, Moser EI, Moser MB (Aug 2006). "Path integration and the neural basis of the 'cognitive map'". Nature Reviews. Neuroscience. 7 (8): 663–78. doi:10.1038/nrn1932. PMID 16858394.
- Mizunami M, Weibrecht JM, Strausfeld NJ (Dec 1998). "Mushroom bodies of the cockroach: their participation in place memory". The Journal of Comparative Neurology. 402 (4): 520–37. doi:10.1002/(SICI)1096-9861(19981228)402:4<520::AID-CNE6>3.0.CO;2-K. PMID 9862324.
- Morris RG, Garrud P, Rawlins JN, O'Keefe J (Jun 1982). "Place navigation impaired in rats with hippocampal lesions". Nature. 297 (5868): 681–83. Bibcode:1982Natur.297..681M. doi:10.1038/297681a0. PMID 7088155.
- Moser MB, Moser EI (1998). "Functional differentiation in the hippocampus". Hippocampus. 8 (6): 608–19. doi:10.1002/(SICI)1098-1063(1998)8:6<608::AID-HIPO3>3.0.CO;2-7. PMID 9882018.
- Moser EI, Kropff E, Moser MB (2008). "Place cells, grid cells, and the brain's spatial representation system". Annual Review of Neuroscience. 31: 69–89. doi:10.1146/annurev.neuro.31.061307.090723. PMID 18284371.
- Nadel L, O'Keefe J, Black A (Jun 1975). "Slam on the brakes: a critique of Altman, Brunner, and Bayer's response-inhibition model of hippocampal function". Behavioral Biology. 14 (2): 151–62. doi:10.1016/S0091-6773(75)90148-0. PMID 1137539.
- Nakazawa K, McHugh TJ, Wilson MA, Tonegawa S (May 2004). "NMDA receptors, place cells and hippocampal spatial memory". Nature Reviews. Neuroscience. 5 (5): 361–72. doi:10.1038/nrn1385. PMID 15100719.
- Nieuwenhuys, R (1982). "An Overview of the Organization of the Brain of Actinopterygian Fishes". Am. Zool. 22 (2): 287–310. doi:10.1093/icb/22.2.287.
- O'Kane G, Kensinger EA, Corkin S (2004). "Evidence for semantic learning in profound amnesia: an investigation with patient H.M". Hippocampus. 14 (4): 417–25. doi:10.1002/hipo.20005. PMID 15224979.
- O'Keefe J, Dostrovsky J (Nov 1971). "The hippocampus as a spatial map. Preliminary evidence from unit activity in the freely-moving rat". Brain Research. 34 (1): 171–75. doi:10.1016/0006-8993(71)90358-1. PMID 5124915.
- O'Keefe J, Nadel L (1978). The Hippocampus as a Cognitive Map. Oxford University Press.
- Portavella M, Vargas JP, Torres B, Salas C (2002). "The effects of telencephalic pallial lesions on spatial, temporal, and emotional learning in goldfish". Brain Research Bulletin. 57 (3–4): 397–99. doi:10.1016/S0361-9230(01)00699-2. PMID 11922997.
- Pearce JM (Sep 2001). "Ammon's horn and the hippocampus". Journal of Neurology, Neurosurgery, and Psychiatry. 71 (3): 351. doi:10.1136/jnnp.71.3.351. PMC 1737533. PMID 11511709.
- Pothuizen HH, Zhang WN, Jongen-Rêlo AL, Feldon J, Yee BK (Feb 2004). "Dissociation of function between the dorsal and the ventral hippocampus in spatial learning abilities of the rat: a within-subject, within-task comparison of reference and working spatial memory". The European Journal of Neuroscience. 19 (3): 705–712. doi:10.1111/j.0953-816X.2004.03170.x. PMID 14984421.
- Prull MW, Gabrieli JD, Bunge SA (2000). "Ch 2. Age-related changes in memory: A cognitive neuroscience perspective". In Craik FI, Salthouse TA. The handbook of aging and cognition. Erlbaum. ISBN 978-0-8058-2966-2.
- Rodríguez F, López JC, Vargas JP, Broglio C, Gómez Y, Salas C (2002). "Spatial memory and hippocampal pallium through vertebrate evolution: insights from reptiles and teleost fish". Brain Research Bulletin. 57 (3–4): 499–503. doi:10.1016/S0361-9230(01)00682-7. PMID 11923018.
- Rolls ET, Xiang JZ (2006). "Spatial view cells in the primate hippocampus and memory recall". Reviews in the Neurosciences. 17 (1–2): 175–200. doi:10.1515/REVNEURO.2006.17.1-2.175. PMID 16703951.
- Rosenzweig ES, Barnes CA (Feb 2003). "Impact of aging on hippocampal function: plasticity, network dynamics, and cognition". Progress in Neurobiology. 69 (3): 143–79. doi:10.1016/S0301-0082(02)00126-0. PMID 12758108.
- Scoville WB, Milner B (Feb 1957). "Loss of recent memory after bilateral hippocampal lesions". Journal of Neurology, Neurosurgery, and Psychiatry. 20 (1): 11–21. doi:10.1136/jnnp.20.1.11. PMC 497229. PMID 13406589.
- Shettleworth SJ (2003). "Memory and hippocampal specialization in food-storing birds: challenges for research on comparative cognition". Brain, Behavior and Evolution. 62 (2): 108–16. doi:10.1159/000072441. PMID 12937349.
- Skaggs WE, McNaughton BL, Wilson MA, Barnes CA (1996). "Theta phase precession in hippocampal neuronal populations and the compression of temporal sequences". Hippocampus. 6 (2): 149–76. doi:10.1002/(SICI)1098-1063(1996)6:2<149::AID-HIPO6>3.0.CO;2-K. PMID 8797016.
- Skaggs WE, McNaughton BL, Permenter M, Archibeque M, Vogt J, Amaral DG, Barnes CA (Aug 2007). "EEG sharp waves and sparse ensemble unit activity in the macaque hippocampus". Journal of Neurophysiology. 98 (2): 898–910. doi:10.1152/jn.00401.2007. PMID 17522177.
- Sloviter RS (Feb 2005). "The neurobiology of temporal lobe epilepsy: too much information, not enough knowledge". Comptes Rendus Biologies. 328 (2): 143–53. doi:10.1016/j.crvi.2004.10.010. PMID 15771000.
- Smith DM, Mizumori SJ (2006). "Hippocampal place cells, context, and episodic memory". Hippocampus. 16 (9): 716–29. CiteSeerX 10.1.1.141.1450. doi:10.1002/hipo.20208. PMID 16897724.
- Solstad T, Boccara CN, Kropff E, Moser MB, Moser EI (Dec 2008). "Representation of geometric borders in the entorhinal cortex". Science. 322 (5909): 1865–68. Bibcode:2008Sci...322.1865S. doi:10.1126/science.1166466. PMID 19095945.
- Squire LR (Apr 1992). "Memory and the hippocampus: a synthesis from findings with rats, monkeys, and humans". Psychological Review. 99 (2): 195–231. doi:10.1037/0033-295X.99.2.195. PMID 1594723.
- Squire LR, Schacter DL (2002). The Neuropsychology of Memory. Guilford Press.
- Squire LR (Jan 2009). "The legacy of patient H.M. for neuroscience". Neuron. 61 (1): 6–9. doi:10.1016/j.neuron.2008.12.023. PMC 2649674. PMID 19146808.
- Sutherland GR, McNaughton B (Apr 2000). "Memory trace reactivation in hippocampal and neocortical neuronal ensembles". Current Opinion in Neurobiology. 10 (2): 180–86. doi:10.1016/S0959-4388(00)00079-9. PMID 10753801.
- Sutherland RJ, Kolb B, Whishaw IQ (Aug 1982). "Spatial mapping: definitive disruption by hippocampal or medial frontal cortical damage in the rat". Neuroscience Letters. 31 (3): 271–6. doi:10.1016/0304-3940(82)90032-5. PMID 7133562.
- Sutherland RJ, Weisend MP, Mumby D, Astur RS, Hanlon FM, Koerner A, Thomas MJ, Wu Y, Moses SN, Cole C, Hamilton DA, Hoesing JM (2001). "Retrograde amnesia after hippocampal damage: recent vs. remote memories in two tasks". Hippocampus. 11 (1): 27–42. doi:10.1002/1098-1063(2001)11:1<27::AID-HIPO1017>3.0.CO;2-4. PMID 11261770.
- Suzuki M, Hagino H, Nohara S, Zhou SY, Kawasaki Y, Takahashi T, Matsui M, Seto H, Ono T, Kurachi M (Feb 2005). "Male-specific volume expansion of the human hippocampus during adolescence". Cerebral Cortex. 15 (2): 187–93. doi:10.1093/cercor/bhh121. PMID 15238436.
- Vanderwolf CH (Dec 2001). "The hippocampus as an olfacto-motor mechanism: were the classical anatomists right after all?". Behavioural Brain Research. 127 (1–2): 25–47. doi:10.1016/S0166-4328(01)00354-0. PMID 11718883.
- Vargas JP, Bingman VP, Portavella M, López JC (Nov 2006). "Telencephalon and geometric space in goldfish". The European Journal of Neuroscience. 24 (10): 2870–78. doi:10.1111/j.1460-9568.2006.05174.x. PMID 17156211.
- VanElzakker M, Fevurly RD, Breindel T, Spencer RL (Dec 2008). "Environmental novelty is associated with a selective increase in Fos expression in the output elements of the hippocampal formation and the perirhinal cortex". Learning & Memory. 15 (12): 899–908. doi:10.1101/lm.1196508. PMC 2632843. PMID 19050162.
- Wechsler RT, Morss, AM, Wustoff, CJ, & Caughey, AB (2004). Blueprints notes & cases: Neuroscience. Oxford: Blackwell Publishing. p. 37. ISBN 978-1-4051-0349-7.
- West MJ (1990). "Stereological studies of the hippocampus: a comparison of the hippocampal subdivisions of diverse species including hedgehogs, laboratory rodents, wild mice and men". Progress in Brain Research. 83: 13–36. doi:10.1016/S0079-6123(08)61238-8. ISBN 9780444811493. PMID 2203095.
- Wilson MA, McNaughton BL (Jul 1994). "Reactivation of hippocampal ensemble memories during sleep". Science. 265 (5172): 676–79. Bibcode:1994Sci...265..676W. doi:10.1126/science.8036517. PMID 8036517.
- Winson J (Jul 1978). "Loss of hippocampal theta rhythm results in spatial memory deficit in the rat". Science. 201 (4351): 160–63. Bibcode:1978Sci...201..160W. doi:10.1126/science.663646. PMID 663646.
Further reading
Journals
- Hippocampus (Wiley)
Books
- Anderson P, Morris R, Amaral, Bliss T, O'Keefe J, eds. (2007). The Hippocampus Book. Oxford University Press. ISBN 978-0-19-510027-3.
- Derdikman D, Knierim JJ, eds. (2014). Space, Time and Memory in the Hippocampal Formation. Springer. ISBN 978-3-7091-1292-2.
- Duvernoy HM, Cattin F (2005). The Human Hippocampus: Functional Anatomy, Vascularization, and Serial Sections with MRI. Springer. ISBN 978-3-540-23191-2.
- Eichenbaum H (2002). The Cognitive Neuroscience of Memory. Oxford University Press US. ISBN 978-0-19-514175-7.
- Sharp PE, ed. (2002). The Neural Basis of Navigation: Evidence from Single Cell Recording. Springer. ISBN 978-0-7923-7579-1.
- Taupin P (2007). The Hippocampus: Neurotransmission and Plasticity in the Nervous System. Nova Publishers. ISBN 978-1-60021-914-6.
- Byrne JH, ed. (2008). Learning and Memory: A comprehensive reference. Elsevier. ISBN 978-0-12-370509-9.
External links
Wikimedia Commons has media related to Hippocampus. |
- Stained brain slice images which include the "hippocampus" at the BrainMaps project
- Diagram of a Hippocampal Brain Slice
- Hippocampus – Cell Centered Database
- Temporal-lobe.com An interactive diagram of the rat parahippocampal-hippocampal region
- Search Hippocampus on BrainNavigator via BrainNavigator
- Buzsaki G (2010). "Hippocampus". Scholarpedia. 6 (1): 1468. Bibcode:2011SchpJ...6.1468B. doi:10.4249/scholarpedia.1468.
No comments:
Post a Comment