AP-1 Transcription Factors Mediate BDNF-Positive Feedback Loop in Cortical Neurons

Tuvikene, Jürgen; Pruunsild, Priit; Orav, Ester; Esvald, Eli‐Eelika; Timmusk, Tõnis

doi:10.1523/jneurosci.3360-15.2016

Cited by 75 publications

(85 citation statements)

References 73 publications

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“…7a). A major target of TrkB signalling is BDNF itself, the expression of which has recently been found to be under the control of a TrkB-mediated positive feedback loop474849. Thus, if AP-2 loss indeed impairs TrkB signalling one would expect the expression of BDNF to be reduced in KO mice lacking neuronal AP-2.…”

Section: Resultsmentioning

confidence: 99%

“…7v,w). Given the positive feedback loop between TrkB signalling and BDNF expression474849, we analysed BDNF mRNA expression levels in WT and AP-2 KO neurons by qPCR (Fig. 7d).…”

Section: Resultsmentioning

confidence: 99%

“…As retrograde transport of TrkB-containing endosomes is required for neurotrophins to exert their transcriptional regulation of activity-dependent genes, most notably of BDNF (ref. 49), in the nucleus3848, the loss of neuronal complexity and subsequent neurodegeneration in AP-2 KO mice is likely the consequence of defective BDNF gene transcriptional regulation due to impaired retrograde autophagosome transport (Fig. 7a).…”

Section: Resultsmentioning

confidence: 99%

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Retrograde transport of TrkB-containing autophagosomes via the adaptor AP-2 mediates neuronal complexity and prevents neurodegeneration

et al. 2017

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Autophagosomes primarily mediate turnover of cytoplasmic proteins or organelles to provide nutrients and eliminate damaged proteins. In neurons, autophagosomes form in distal axons and are trafficked retrogradely to fuse with lysosomes in the soma. Although defective neuronal autophagy is associated with neurodegeneration, the function of neuronal autophagosomes remains incompletely understood. We show that in neurons, autophagosomes promote neuronal complexity and prevent neurodegeneration in vivo via retrograde transport of brain-derived neurotrophic factor (BDNF)-activated TrkB receptors. p150Glued/dynactin-dependent transport of TrkB-containing autophagosomes requires their association with the endocytic adaptor AP-2, an essential protein complex previously thought to function exclusively in clathrin-mediated endocytosis. These data highlight a novel non-canonical function of AP-2 in retrograde transport of BDNF/TrkB-containing autophagosomes in neurons and reveal a causative link between autophagy and BDNF/TrkB signalling.

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Section: Resultsmentioning

confidence: 99%

“…7v,w). Given the positive feedback loop between TrkB signalling and BDNF expression474849, we analysed BDNF mRNA expression levels in WT and AP-2 KO neurons by qPCR (Fig. 7d).…”

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Retrograde transport of TrkB-containing autophagosomes via the adaptor AP-2 mediates neuronal complexity and prevents neurodegeneration

et al. 2017

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“…BDNF promoter constructs were generated by amplifying the corresponding sequences from rat genomic DNA using the Expand High Fidelity PCR System (Roche) and cloning into pGL4.15[luc2P/Hygro] (Promega) in front of the firefly luciferase coding sequence. Rat and human BDNF promoter IV and VI constructs have been described previously: rat IV (Koppel & Timmusk, ), human IV (Pruunsild et al, ), rat and human VI (Tuvikene, Pruunsild, Orav, Esvald, & Timmusk, ). Genome Browser coordinates for the used genomic fragments are as follows: rat IV chr3:100,786,659‐100,787,183/rn6, rat VI chr3:100,787,725‐100,788,266/rn6, human IV chr11:27,701,313‐27,701,837/hg38, human VI chr11:27,700,200‐27,700,772/hg38.…”

Section: Methodsmentioning

confidence: 99%

Dopamine cross‐reacts with adrenoreceptors in cortical astrocytes to induce BDNF expression, CREB signaling and morphological transformation

Koppel

Jaanson

Klasche

et al. 2017

Glia

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Expression of brain-derived neurotrophic factor (BDNF) is induced in cultured rat cortical astrocytes by catecholamines norepinephrine and dopamine as well as selective a1 and b adrenergic agonists. However, it has remained unknown which receptors mediate dopamine-induced BDNF upregulation in astrocytes. Here, we demonstrate that b adrenoreceptors are the main mediators of this effect in cultured cortical astrocytes, while a1 adrenoreceptors and D1 dopamine receptors contribute to a lesser extent. We show that in cortical astrocytes BDNF exon IV and exon VI containing mRNAs are induced by dopamine and norepinephrine via CREB-dependent signaling and that this regulation is mediated by a mechanism that is distinct from activity-dependent CREBmediated activation of BDNF transcription in neurons. We also show that regulation of BDNF promoters IV and VI by catecholamines requires a distal regulatory element in the BDNF locus.Finally, we demonstrate that dopamine-induced astrocyte stellation and induction of CREB signaling are mediated by cross-reaction of dopamine with b adrenoreceptors.

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“…c-Jun can associate with another transcription factor, c-Fos, to form the AP-1 transcriptional complex, which can in turn regulate the expression of several genes including those related to cell cycle progression and differentiation [19]. Intriguingly, AP-1 transcription factors are critical for positive feedback loops induced by brain derived neurotrophic factor (BDNF) in cortical neurons [22], a growth factor critical for long-lasting memory and plasticity (reviewed below). Moreover, AP-1 DNA binding activity is increased after LTP induction in the dentate gyrus [23], and a specific inhibitor of JNK phosphorylation, but not ERK1/2 or p38 MAPK phosphorylation, enhanced STM and blocked LTM for inhibitory avoidance in rats [24].…”

Section: Spatially- and Temporally-regulated Molecular Signaling Imentioning

confidence: 99%

The Contribution of Spatial and Temporal Molecular Networks in the Induction of Long-term Memory and Its Underlying Synaptic Plasticity

Mirisis¹,

Alexandrescu²,

Carew³

et al. 2016

AIMS Neuroscience

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The ability to form long-lasting memories is critical to survival and thus is highly conserved across the animal kingdom. By virtue of its complexity, this same ability is vulnerable to disruption by a wide variety of neuronal traumas and pathologies. To identify effective therapies with which to treat memory disorders, it is critical to have a clear understanding of the cellular and molecular mechanisms which subserve normal learning and memory. A significant challenge to achieving this level of understanding is posed by the wide range of distinct temporal and spatial profiles of molecular signaling induced by learning-related stimuli. In this review we propose that a useful framework within which to address this challenge is to view the molecular foundation of long-lasting plasticity as composed of unique spatial and temporal molecular networks that mediate signaling both within neurons (such as via kinase signaling) as well as between neurons (such as via growth factor signaling). We propose that evaluating how cells integrate and interpret these concurrent and interacting molecular networks has the potential to significantly advance our understanding of the mechanisms underlying learning and memory formation.

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AP-1 Transcription Factors Mediate BDNF-Positive Feedback Loop in Cortical Neurons

Cited by 75 publications

References 73 publications

Retrograde transport of TrkB-containing autophagosomes via the adaptor AP-2 mediates neuronal complexity and prevents neurodegeneration

Retrograde transport of TrkB-containing autophagosomes via the adaptor AP-2 mediates neuronal complexity and prevents neurodegeneration

Dopamine cross‐reacts with adrenoreceptors in cortical astrocytes to induce BDNF expression, CREB signaling and morphological transformation

The Contribution of Spatial and Temporal Molecular Networks in the Induction of Long-term Memory and Its Underlying Synaptic Plasticity

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