Correlation between long‐term potentiation and release of endogenous amino acids from dentate gyrus of anaesthetized rats.

Bliss, T. V. P.; Douglas, R. M.; Er̀rington, M.L.; Lynch, Marina A.

doi:10.1113/jphysiol.1986.sp016193

Cited by 287 publications

(72 citation statements)

References 44 publications

(51 reference statements)

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“…Furthermore the experiments of Bliss and co-workers indicate that LTP is maintained, at least in part, by a sustained increase in transmitter (e.g. glutamate) release (Bliss et al, 1988(Bliss et al, , 1986Errington et al, 1987;Lynch et al, 1989a). These findings were challenged by Ben-Ari and co-workers (Anikszteijn et al, 1989(Anikszteijn et al, , 1991, but confirmed by recent observations in our group (Ghijsen and Lopes da Ghijsen et al, 1992).…”

Section: Introductionsupporting

confidence: 74%

Presynaptic plasticity: The regulation of Ca2+-dependent transmitter release

Verhage

Ghijsen

Silva

1994

Progress in Neurobiology

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Section: Introductionsupporting

confidence: 74%

Presynaptic plasticity: The regulation of Ca2+-dependent transmitter release

Verhage

Ghijsen

Silva

1994

Progress in Neurobiology

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“…Thus, there is evidence to support modifications presynaptically (Bliss et al, 1986;Malgaroli and Tsien, 1992;Bolshakov and Seigelbaum, 1994;Stevens and Wang, 1994), postsynaptically (Davies et al, 1989;Zalutsky and Nicoll, 1990;Manabe et al, 1992;Isaac et al, 1995;Liao et al, 1995;Oliet et al, 1996), and even on different postsynaptic receptors (Muller and Lynch, 1988;Kullman, 1994;Selig et al, 1995). Our experiments suggest that these modifications are maintained by autonomous PKC phosphorylation that is increased or decreased by the pattern of ongoing afferent activity.…”

Section: Pkm and The Divergence And Convergence Of Signal Transductiomentioning

confidence: 53%

Bidirectional Regulation of Protein Kinase Mζ in the Maintenance of Long-Term Potentiation and Long-Term Depression

1996

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Long-term potentiation (LTP) and long-term depression (LTD) are persistent modifications of synaptic efficacy that may contribute to information storage in the CA1 region of the hippocampus. Persistently enhanced phosphorylation has been implicated in the maintenance phase of LTP. This hypothesis is supported by our previous observation that protein kinase M (PKM), the constitutively active catalytic fragment of a single protein kinase C isoform (PKC), increases in LTP maintenance. In contrast, dephosphorylation may be important in LTD maintenance, because phosphatase inhibitors reverse established LTD, in addition to blocking its induction. Because phosphorylation is determined by a balance of phosphatases and kinases, both increases in phosphatase activity and decreases in kinase activity could contribute to LTD. We now report that the reduction of protein kinase activity by H7, as well as selective inhibition of PKC by chelerythrine, mimics and occludes the maintenance phase of homosynaptic LTD in rat hippocampal slices. Conversely, saturated LTD occludes the synaptic depression caused by chelerythrine. Biochemical analysis demonstrates a decrease of PKM, as well as PKCs ␥ and ⑀, in LTD maintenance and a concomitant loss of constitutive PKC activity. LTD and the downregulation of PKM are prevented by NMDA receptor antagonists and Ca 2ϩ -dependent protease inhibitors. Both LTD and the downregulation of PKM are reversible by high-frequency afferent stimulation. Our findings indicate that the molecular mechanisms of LTP and LTD maintenance are inversely related through the bidirectional regulation of PKC.

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“…The mechanism could involve presynaptic changes (increased glutamate release), postsynaptic changes (increased number of AMPA receptors or changes of the binding properties of AMPA receptors), or glial changes (reduced uptake of glutamate by glial cells) [Bindman et al, 19911. Indeed, the issue is complex because there is evidence in favor of all these changes, some of it contradictory [Bliss et al, 1986;Foster and McNaughton, 1991;Tsumoto, 1992;Voronin, 19891. At this time, perhaps the most favored hypothesis is that LTP is maintained through a combination of pre-and postsynaptic mechanisms, a combination which may be different in different synapses and that might, in some, include morphological or extrasynaptic changes [Bindman et al, 1991;Bliss and Collingridge, 1993;Colley and Routtenberg, 1993;Hawkins et al, 19931. There is now little doubt that protein phosphorylation, perhaps of glutamatergic receptors, and perhaps mainly through the intervention of PKC, is crucial for the first 3 or so hours of the maintenance phase [Colley and Routtenberg, 1993;Reymann et al, 19881, and that later other mechanisms enter into play, like protein synthesis and gene expression [see Colley and Routtenberg, 1993;Sheu et al, 19931. After 3 h, LTP can be blocked by protein synthesis inhibitors, the best studied of which is anisomycin applied to CA1 slices [Frey et al, 19881 or to the dentate gyrus in freely moving rats [Matthies, 19891.…”

Section: Ltp Maintenancementioning

confidence: 99%

Long‐term potentiation and the mechanisms of memory

Izquierdo

1993

Drug Development Research

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Long-term potentiation (LIP) is a cellular model of the memory processes that occurs in many nerve cells, usually at glutamatergic synapses. For this reason, glutamatergic synapses being the most abundant in the brain, LTP has been widely proposed as a mechanism of memory. Recent findings support this proposal and indicate that, indeed, LTP and memory processes share many properties. The initial steps of LTP and of memory involve the activation of glutamatergic NMDA (N-methyl-D-asprtate) receptors, sensitive to AP5 (amino phosphono valerate), and are very sensitive to inhibition by GABA, (gamma amino butyric acid type A) receptor agonists. The phase that follows in the next 2 or 3 h depends on activation of protein kinase C (PKC) and is sensitive to inhibitors of this enzyme family. Like LTP, the underlying mechanism of memories persists for very long periods without the need of expression; and, like LTP, memories are readily expressed upon a reinstatement of the stimuli used in their induction, as i s the case in test sessions. The expression of LTP and the expression of memory rely on AMPA (D,L-alpha-amino hydroxy methyl isoxazolone propionate) receptors sensitive to CNQX (cyano nitro quinoxaline dione). LTP occurs in many places within the brain, including the hippocampus, amygala, medial septum, and entorhinal cortex. The drug effects on memory mentioned above are seen when the drugs are infused into these brain regions. The region(s) involved depend on the type of memory being processed. These findings support the idea that LTP underlies memory acquisition, retention, and retrieval (the latter, at least for many days after acquisition) and may provide some clues for the development of drugs to alleviate memory disorders. o 1993 Wiley-Liss, Inc.

show abstract

Correlation between long‐term potentiation and release of endogenous amino acids from dentate gyrus of anaesthetized rats.

Cited by 287 publications

References 44 publications

Presynaptic plasticity: The regulation of Ca2+-dependent transmitter release

Presynaptic plasticity: The regulation of Ca2+-dependent transmitter release

Bidirectional Regulation of Protein Kinase Mζ in the Maintenance of Long-Term Potentiation and Long-Term Depression

Long‐term potentiation and the mechanisms of memory

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