Tissue plasminogen activator controls multiple forms of synaptic plasticity and memory

Calabresi, Paolo; Napolitano, Maddalena; Centonze, Diego; Marfia, Girolama Alessandra; Gubellini, Paolo; Ammassari–Teule, Martine; Berretta, Nicola; Bernardi, Giorgio; Frati, Luigi; Tolu, Massimo; Gulino, Alberto

doi:10.1046/j.1460-9568.2000.00991.x

Cited by 163 publications

(142 citation statements)

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“…In the brain parenchyma, tPA interactions extend beyond plasminogen to the NMDAR in the control of functions such as learning processes in the hippocampus (LTP and LTD) [24][25][26] and dysfunctions such as neurotoxicity. 7,27 Our present data set emphasize the role of tPA molecular form on its interaction with NMDAR in different structures of the central nervous system (CNS).…”

Section: Discussionmentioning

confidence: 99%

Unveiling an exceptional zymogen: the single-chain form of tPA is a selective activator of NMDA receptor-dependent signaling and neurotoxicity

et al. 2012

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Section: Discussionmentioning

confidence: 99%

Unveiling an exceptional zymogen: the single-chain form of tPA is a selective activator of NMDA receptor-dependent signaling and neurotoxicity

et al. 2012

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“…t-PA is an extracellular serine protease that is expressed after LTP induction and released after local mGluR-dependent synthesis (28,29). Proteolytic activity of t-PA is necessary for experience-dependent synaptic pruning, LTP consolidation, and the formation of perforated synaptic profiles (30). Levels of SERBP1, an mRNA-binding protein mediating cyclic nucleotide destabilization of the mRNA encoding the major endogenous inhibitor of t-PA, PAI-1 (31), were up-regulated.…”

Section: Discussionmentioning

confidence: 99%

Quantitative proteomic analysis of primary neurons reveals diverse changes in synaptic protein content in fmr1 knockout mice

Liao¹,

Park²,

Xu³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

159

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Fragile X syndrome (FXS) is a common inherited form of mental retardation that is caused, in the vast majority of cases, by the transcriptional silencing of a single gene, fmr1. The encoded protein, FMRP, regulates mRNA translation in neuronal dendrites, and it is thought that changes in translation-dependent forms of synaptic plasticity lead to many symptoms of FXS. However, little is known about the potentially extensive changes in synaptic protein content that accompany loss of FMRP. Here, we describe the development of a high-throughput quantitative proteomic method to identify differences in synaptic protein expression between wild-type and fmr1؊/؊ mouse cortical neurons. The method is based on stable isotope labeling by amino acids in cell culture (SILAC), which has been used to characterize differentially expressed proteins in dividing cells, but not in terminally differentiated cells because of reduced labeling efficiency. To address the issue of incomplete labeling, we developed a mathematical method to normalize protein ratios relative to a reference based on the labeling efficiency. Using this approach, in conjunction with multidimensional protein identification technology (MudPIT), we identified >100 proteins that are up-or down-regulated. These proteins fall into a variety of functional categories, including those regulating synaptic structure, neurotransmission, dendritic mRNA transport, and several proteins implicated in epilepsy and autism, two endophenotypes of FXS. These studies provide insights into the potential origins of synaptic abnormalities in FXS and a demonstration of a methodology that can be used to explore neuronal protein changes in neurological disorders. stable isotope labeling ͉ proteomics ͉ mass spectrometry ͉ fragile X syndrome F ragile X syndrome (FXS) is the most common inherited form of mental retardation. It is characterized by low IQ (1) and a broad set of symptoms other than retardation that compound the level of impairment. These include autistic spectrum behaviors, attention deficit and hyperactivity, childhood seizures, and several physical manifestations (2, 3). The most profound neuroanatomical abnormality seen in the brains of FXS patients is a preponderance of long, thin, and ''tortuous'' dendritic spines in cortex (4). This cortical phenotype is recapitulated in the fmr1 knockout (KO) mouse model, which also exhibits abnormal spine morphologies in the hippocampus and cerebellum (5, 6).In the vast majority of cases, FXS is caused by expansion of a trinucleotide repeat (CGG) within the 5Ј-untranslated region of the X-linked gene fmr1, resulting in its transcriptional silencing. The encoded protein, FMRP, can act as a translational suppressor of mRNAs in dendrites, controlling the localized, activity-dependent expression of a potentially large subset of synaptic proteins (7). Knocking out fmr1 in mouse results in a perturbation of various forms of translation-dependent synaptic plasticity, including some forms of long-term potentiation (LTP) and group I metabotropic...

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“…Additionally, early phases of instrumental learning (Hernandez et al 2006;Kelly and Deadwyler 2003) elicit widespread zif/268 and arc induction throughout an extensive corticostriatal network in rats. Furthermore, knockdown of c-fos, zif/268, arc, or tissue plasminogen activator (tPA) that cleaves proBDNF to mature BDNF impairs longterm memory consolidation (Calabresi et al 2000, Guzowski et al 2000Fleischmann et al 2003;Jones et al 2001 and produces deficits in drug-induced conditioned place preference (Valjent et al 2006). …”

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confidence: 99%

Relapse to cocaine seeking increases activity-regulated gene expression differentially in the prefrontal cortex of abstinent rats

et al. 2008

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Rationale-Alterations in the activity of the prefrontal and orbitofrontal cortices of cocaine addicts have been linked with re-exposure to cocaine-associated stimuli. Objectives Using an animal model of relapse to cocaine seeking, the present study investigated the expression patterns of four different activity-regulated genes within prefrontal cortical brain regions after 22 h or 15 days of abstinence during context-induced relapse.Materials and methods-Rats self-administered cocaine or received yoked-saline for 2 h/day for 10 days followed by 22 h or 2 weeks of abstinence when they were re-exposed to the selfadministration chamber with or without levers available to press for 1 h. Brains were harvested and sections through the prefrontal cortex were processed for in situ hybridization using radioactive oligonucleotide probes encoding c-fos, zif/268, arc, and bdnf.Results-Re-exposure to the chamber in which rats previously self-administered cocaine but not saline, regardless of lever availability, increased the expression of all genes in the medial prefrontal and orbitofrontal cortices at both time points with one exception: bdnf mRNA was significantly increased in the medial prefrontal cortex at 22 h only if levers previously associated with cocaine delivery were available to press. Furthermore, re-exposure of rats to the chambers in which they received yoked saline enhanced both zif/268 and arc expression selectively in the orbito-frontal cortex after 15 days of abstinence.Correspondence to: J. F. McGinty. HHS Public AccessAuthor manuscript Psychopharmacology (Berl). Author manuscript; available in PMC 2017 May 22. Author Manuscript Author ManuscriptAuthor Manuscript Author ManuscriptConclusions-These results support convergent evidence that cocaine-induced changes in the prefrontal cortex are important in regulating drug seeking following abstinence and may provide additional insight into the molecular mechanisms involved in these processes. KeywordsAddiction; Arc; BDNF; c-fos; Relapse; zif/268; Self-administration; Abstinence; ExtinctionRelapse to drug seeking and taking in addicted humans is often triggered by re-exposure to environmental cues previously associated with the drug (Ehrman et al. 1992). Similarly, in animal studies, during chronic drug self-administration, the drug-paired environment acquires conditioned reinforcing properties that trigger drug-seeking behavior upon reexposure to the context following forced abstinence (Crombag and Shaham 2002;Fuchs et al. 2005Fuchs et al. , 2006. Thus, like other forms of learning, relapse to drug-seeking involves the formation and retrieval of instrumental memories (Hyman 2005). A major question in addiction research is whether the neural substrates underlying drug-seeking involve the same cell signaling and synaptic plasticity processes within the same brain regions as those implicated in other forms of reward learning and memory (Berke and Hyman 2000;Hyman and Malenka 2001;Nestler 2001).The inhibitory control functions of the prefrontal cortical ...

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Tissue plasminogen activator controls multiple forms of synaptic plasticity and memory

Cited by 163 publications

References 60 publications

Unveiling an exceptional zymogen: the single-chain form of tPA is a selective activator of NMDA receptor-dependent signaling and neurotoxicity

Unveiling an exceptional zymogen: the single-chain form of tPA is a selective activator of NMDA receptor-dependent signaling and neurotoxicity

Quantitative proteomic analysis of primary neurons reveals diverse changes in synaptic protein content in fmr1 knockout mice

Relapse to cocaine seeking increases activity-regulated gene expression differentially in the prefrontal cortex of abstinent rats

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