Epigenetic Priming of Memory Updating during Reconsolidation to Attenuate Remote Fear Memories

Gräff, Johannes; Joseph, Naima T.; Horn, Meryl E.; Samiei, Alireza; Meng, Jia; Seo, Jinsoo; Rei, Damien; Bero, Adam W.; Phan, Trongha; Wagner, Florence F.; Holson, Edward B.; Xu, Jinbin; Sun, Jianjun; Neve, Rachael L.; Mach, Robert H.; Haggarty, Stephen J.; Tsai, Li Huei

doi:10.1016/j.cell.2013.12.020

Cited by 323 publications

(340 citation statements)

References 70 publications

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“…It is currently not clear whether this within-session extinction also persists between sessions, but this would be worthy of future investigation. Consistent with this suggestion, previous research has shown that inhibition of Class I HDACs can enhance fear extinction memory (Bahari-Javan et al, 2012;Bredy and Barad, 2008;Graff et al, 2014;Lattal et al, 2007;Stafford et al, 2012;Whittle et al, 2013). Although systemic pharmacological HDAC3 inhibition fails to enhance cued fear extinction (Bowers et al, 2015), site-specific HDAC3 inhibition restricted to the hippocampus or amygdala might reveal an important role of HDAC3 in fear extinction memory.…”

Section: Discussionsupporting

confidence: 62%

Context and Auditory Fear are Differentially Regulated by HDAC3 Activity in the Lateral and Basal Subnuclei of the Amygdala

Kwapis

Alaghband

López

et al. 2016

Neuropsychopharmacol

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Histone acetylation is a fundamental epigenetic mechanism that is dynamically regulated during memory formation. Histone acetyltransferases (HATs) and histone deacetylases (HDACs) compete to modulate histone acetylation, allowing for rapid changes in acetylation in response to a learning event. HDACs are known to be powerful negative regulators of memory formation, but it is not clear whether this function depends on HDAC enzymatic activity per se. Here, we tested whether the enzymatic activity of an individual Class I HDAC, HDAC3, has a role in fear memory formation in subregions of the hippocampus and amygdala. We found that fear conditioning drove expression of the immediate early genes cFos and Nr4a2 in the hippocampus, which coincided with reduced HDAC3 occupancy at these promoters. Using a dominant-negative, deacetylase-dead point mutant virus (AAV-HDAC3(Y298H)-v5), we found that selectively blocking HDAC3 deacetylase activity in either the dorsal hippocampus or basal nucleus of the amygdala enhanced context fear without affecting tone fear. Blocking HDAC3 activity in the lateral nucleus of the amygdala, on the other hand, enhanced tone, but not context fear memory. These results show for the first time that the enzymatic activity of HDAC3 functions to negatively regulate fear memory formation. Further, HDAC3 activity regulates different aspects of fear memory in the basal and lateral subregions of the amygdala. Thus, the deacetylase activity of HDAC3 is a powerful negative regulator of fear memory formation in multiple subregions of the fear circuit.

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Section: Discussionsupporting

confidence: 62%

Context and Auditory Fear are Differentially Regulated by HDAC3 Activity in the Lateral and Basal Subnuclei of the Amygdala

Kwapis

Alaghband

López

et al. 2016

Neuropsychopharmacol

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“…All these data suggest that HDAC1 and HDAC2 contribute to the secondary functional loss after stroke. HDAC2 is an isoform negatively regulating cell survival (Nott et al, 2008) and neuronal plasticity (Gräff et al, 2014). In contrast, HDAC1 gain of function has a potent protection effect against neurotoxicity in vivo model for ischemia (Kim et al, 2008).…”

Section: Resultsmentioning

confidence: 99%

“…Histone deacetylases (HDACs) target histones, regulate chromosome dynamics, control cellular gene expression (Robert et al, 2011), and contribute to multiple signaling pathways linked to neuronal plasticity (Gräff et al, 2014), cell survival (Nott et al, 2008), neuroinflammation (Bie et al, 2014), and oxidative stress (Shimazu et al, 2013;Peng et al, 2015). Thus, HDACs may play a critical role in mediating pathophysiological events in the periinfarct area after stroke.…”

Section: Introductionmentioning

confidence: 99%

Opening a New Time Window for Treatment of Stroke by Targeting HDAC2

et al. 2017

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Narrow therapeutic window limits treatments with thrombolysis and neuroprotection for most stroke patients. Widening therapeutic window remains a critical challenge. Understanding the key mechanisms underlying the pathophysiological events in the peri-infarct area where secondary injury coexists with neuroplasticity over days to weeks may offer an opportunity for expanding the therapeutic window. Here we show that ischemia-induced histone deacetylase 2 (HDAC2) upregulation from 5 to 7 d after stroke plays a crucial role. In this window phase, suppressing HDAC2 in the peri-infarct cortex of rodents by HDAC inhibitors, knockdown or knock-out of Hdac2 promoted recovery of motor function from stroke via epigenetically enhancing cells survival and neuroplasticity of surviving neurons as well as reducing neuroinflammation, whereas overexpressing HDAC2 worsened stroke-induced functional impairment of both WT and Hdac2 conditional knock-out mice. More importantly, inhibiting other isoforms of HDACs had no effect. Thus, the intervention by precisely targeting HDAC2 in this window phase is a novel strategy for the functional recovery of stroke survivors.

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“…In the same year, Misanin et al (1968) suggested that consolidated memories become labile and susceptible to modulation when they are reactivated; that is, when they are evoked, they must undergo a new stabilization process to persist (Nader et al 2000;Sara 2000;de la Fuente et al 2011;Gräff et al 2014). This new stabilization process has been termed "reconsolidation" (Przybyslawski et al 1999).…”

Section: [Supplemental Materials Is Available For This Article]mentioning

confidence: 99%

Spermidine-induced improvement of reconsolidation of memory involves calcium-dependent protein kinase in rats

et al. 2015

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In this study, we determined whether the calcium-dependent protein kinase (PKC) signaling pathway is involved in the improvement of fear memory reconsolidation induced by the intrahippocampal administration of spermidine in rats. Male Wistar rats were trained in a fear conditioning apparatus using a 0.4-mA footshock as an unconditioned stimulus. Twenty-four hours after training, animals were re-exposed to the apparatus in the absence of shock (reactivation session). Immediately after the reactivation session, spermidine (2 -200 pmol/site), the PKC inhibitor 3-[1-(dimethylaminopropyl)indol-3-yl]-4-(indol-3-yl) maleimide hydrochloride (GF 109203X, 0.3 -30 pg/site), the antagonist of the polyamine-binding site at the NMDA receptor, arcaine (0.2 -200 pmol/site), or the PKC activator phorbol 12-myristate 13-acetate (PMA, 0.02 -2 nmol/site) was injected. While the post-reactivation administration of spermidine (20 and 200 pmol/site) and PMA (2 nmol/site) improved memory reconsolidation, GF 109203X (1, 10, and 30 pg/site) and arcaine (200 pmol/site) impaired it. GF 109203X (0.3 pg/site) impaired memory reconsolidation in the presence of spermidine (200 pmol/site). PMA (0.2 nmol/site) prevented the arcaine (200 pmol/site)-induced impairment of memory reconsolidation. Anisomycin (2 mg/site) also impaired memory reconsolidation in the presence of spermidine (200 pmol/site). Drugs had no effect when they were administered in the absence of reactivation. These results suggest that the spermidine-induced enhancement of memory reconsolidation involves PKC activation.

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Epigenetic Priming of Memory Updating during Reconsolidation to Attenuate Remote Fear Memories

Cited by 323 publications

References 70 publications

Context and Auditory Fear are Differentially Regulated by HDAC3 Activity in the Lateral and Basal Subnuclei of the Amygdala

Context and Auditory Fear are Differentially Regulated by HDAC3 Activity in the Lateral and Basal Subnuclei of the Amygdala

Opening a New Time Window for Treatment of Stroke by Targeting HDAC2

Spermidine-induced improvement of reconsolidation of memory involves calcium-dependent protein kinase in rats

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