Activin increases the number of synaptic contacts and the length of dendritic spine necks by modulating spinal actin dynamics

Shoji-Kasai, Yoko; Ageta, Hiroshi; Hasegawa, Yoshihisa; Tsuchida, Kunihiro; Sugino, Hiromu; Inokuchi, Kaoru

doi:10.1242/jcs.012450

Cited by 60 publications

(54 citation statements)

References 48 publications

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“…Inactivation of activin receptor in the forebrain enhanced both GABA A and GABA B currents, but whether this requires canonical signaling was not tested. In contrast, in cultured hippocampal neurons, addition of activin results in spine contact and NMDA receptor changes through protein synthesis-independent (noncanonical) phosphorylation of actin filaments and postsynaptic scaffold proteins (Shoji-Kasai et al, 2007;Kurisaki et al, 2008). Our results suggest that Smad4 regulates GABA A transmission; however, since Smad4 represents a point of convergence between TGF-␤/activin and BMP signaling pathways, it is not clear which set of ligands might be involved in this response.…”

Section: Canonical Versus Noncanonical Tgf-␤ Pathway Signaling In Hipcontrasting

confidence: 58%

Canonical TGF-β Signaling Is Required for the Balance of Excitatory/Inhibitory Transmission within the Hippocampus and Prepulse Inhibition of Acoustic Startle

Sun¹,

Gewirtz²,

Bofenkamp³

et al. 2010

J. Neurosci.

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Smad4 is a unique nuclear transducer for all TGF-␤ signaling pathways and regulates gene transcription during development and tissue homeostasis. To elucidate the postnatal role of TGF-␤ signaling in the mammalian brain, we generated forebrain-specific Smad4 knockout mice. Surprisingly, the mutants showed no alteration in long-term potentiation and water maze, suggesting that Smad4 is not required for spatial learning and memory. However, these mutant mice did show enhancement of paired-pulse facilitation in excitatory synaptic transmission and stronger paired-pulse depression of GABA A currents in the hippocampus. The alteration of hippocampal electrophysiology correlated with mouse hyperactivity in homecage and open field tests. Mutant mice also showed overgrooming as well as deficits of prepulse inhibition, a widely used endophenotype of schizophrenia. With a specific real-time PCR array focused on TGF-␤ signaling pathway, we identified a novel regulation mechanism of the pathway in the hippocampal neurons, in which Smad4-mediated signaling suppresses the level of extracellular antagonism of TGF-␤ ligands through transcriptional regulation of follistatin, a selective inhibitor to activin/TGF-␤ signaling in the hippocampus. In summary, we suggest that the canonical TGF-␤ signaling pathway is critical for use-dependent modulation of GABA A synaptic transmission and dendritic homeostasis; furthermore, a disruption in the balance of the excitatory and inhibitory hippocampal network can result in psychiatric-like behavior.

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Section: Canonical Versus Noncanonical Tgf-␤ Pathway Signaling In Hipcontrasting

confidence: 58%

Canonical TGF-β Signaling Is Required for the Balance of Excitatory/Inhibitory Transmission within the Hippocampus and Prepulse Inhibition of Acoustic Startle

Sun¹,

Gewirtz²,

Bofenkamp³

et al. 2010

J. Neurosci.

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“…S9). In relation to dendritic spine morphology, activin increases the spine length of hippocampal neurons in a protein and RNA synthesis-independent manner (36). Therefore, our observation that activin promotes dendritic complexity may represent a late phase phenomenon that occurs after an increase in the number or strength of synaptic contacts that are made during the early phase of response to activin.…”

Section: Discussionmentioning

confidence: 76%

Involvement of the Serum Response Factor Coactivator Megakaryoblastic Leukemia (MKL) in the Activin-regulated Dendritic Complexity of Rat Cortical Neurons*

Ishikawa

Nishijima

Shiota

et al. 2010

Journal of Biological Chemistry

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Dynamic changes in neuronal morphology and transcriptional regulation play crucial roles in the neuronal network and function. Accumulating evidence suggests that the megakaryoblastic leukemia (MKL) family members, which function not only as actin-binding proteins but also as serum response factor (SRF) transcriptional coactivators, regulate neuronal morphology. However, the extracellular ligands and signaling pathways, which activate MKL-mediated morphological changes in neurons, remain unresolved. Here, we demonstrate that in addition to MKL1, MKL2, highly enriched in the forebrain, strongly contributes to the dendritic complexity, and this process is triggered by stimulation with activin, a member of the transforming growth factor ␤ (TGF-␤) superfamily. Activin promoted dendritic complexity in a SRF-and MKL-dependent manner without drastically affecting MKL localization and protein levels. In contrast, activin promoted the nuclear export of suppressor of cancer cell invasion (SCAI), which is a corepressor for SRF and MKL. Furthermore, overexpression of SCAI blocked activin-induced SRF transcriptional responses and dendritic complexity. Collectively, these results strongly suggest that activin-SCAI-MKL signaling is a novel pathway that regulates the dendritic morphology of rat cortical neurons by excluding SCAI from the nucleus and activating MKL/SRF-mediated gene expression. Serum response factor (SRF)4 is a transcription factor that binds to a consensus sequence CC(A/T) 6 GG (called the CArG box), which is present in the promoters of several immediateearly or cytoskeletal genes (1). Several studies have demonstrated that deletion mutants of SRF in the mouse brain result in the attenuation of activity-dependent expression of immediate-early genes, impair synaptic plasticity and learning (2, 3), reduce neurite outgrowth, and show abnormality of pathfindings and neuronal migration (4, 5). These findings strongly suggest that SRF plays an important role in neuronal development and plasticity (6). SRF-dependent transcription is controlled by at least two different types of coactivators. One comprises the ternary complex factors, which mainly regulate the immediateearly genes such as c-fos (7). The other type of coactivator comprises megakaryoblastic leukemia (MKL) family members. The MKL family consists of megakaryocytic acute leukemia/ megakaryoblastic leukemia 1/myocardin-related transcription factor-A/basic SAP, and coiled-coil domain (MAL/MKL1/ MRTF-A/BSAC) and MKL2/MRTF-B (8 -13). In nonneuronal cells, MKL1 is primarily activated by actin rearrangement stimulated with the activation of Rho GTPases; that is, release of MKL1 from G-actin enables MKL1 to translocate to the nucleus where it binds to and activates SRF (14). MKL2, in addition to MKL1, regulates a set of cytoskeletal genes (11, 12). Furthermore, suppressor of cancer cell invasion (SCAI) has recently been identified as an MKL-interacting cofactor that inhibits cancer cell invasion (15). Therefore, SRF-driven transcriptional regulation appears to be ...

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“…Thus, it is feasible that the actin network guarantees the molecular/morphological basis for a tag-related housekeeping process, on top of which other key molecules like CaMKII or MAPK are only able to exert their action in synapses specifically marked either for LTP or LTD processes. Furthermore, the actin network could be involved in the PRP capture process itself by providing a distinct geometry for interactions of the kinases with the PRPs such as sculpting active synaptic zones or the whole synaptic spine, guaranteeing, for example, the activation or transport of PRPs into the spine or the transport of new AMPA-receptors to maintain LTP (Fukazawa et al, 2003;Lisman, 2003;Chen et al, 2007;Shoji-Kasai et al, 2007;Yang et al, 2008;Peng et al, 2009). Alternatively, actin filament formation could also be locally involved in PRP synthesis.…”

Section: Discussionmentioning

confidence: 99%

Interfering with the Actin Network and Its Effect on Long-Term Potentiation and Synaptic Tagging in Hippocampal CA1 Neurons in SlicesIn Vitro

Ramachandran

Frey²

2009

J. Neurosci.

120

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Long-term potentiation (LTP) is a cellular correlate for memory formation, which requires the dynamic changes of the actin cytoskeleton. As shown by others, the polymerization of the actin network is important for early stages of LTP. Here, we investigated the role of actin dynamics in synaptic tagging and particularly in the induction of protein synthesis-dependent late-LTP in the CA1 region in hippocampal slices in vitro. We found that the inhibition of actin polymerization affects protein synthesis-independent early-LTP, prevents late-LTP, and interferes with synaptic tagging in apical dendrites of hippocampal CA1. The transformation of early-LTP into late-LTP was blocked by the application of the structurally different actin polymerization inhibitors latrunculin A or cytochalasin D. We suggest that the actin network is required for early "housekeeping" processes to induce and maintain early-LTP. Furthermore, inhibition of actin dynamics negatively interacts with the setting of the synaptic tagging complex. We propose actin as a further tag-specific molecule in apical CA1 dendrites where it is directly involved in the tagging/capturing machinery. Consequently, inhibition of the actin network prevents the interaction of tagging complexes with plasticity-related proteins. This results in the prevention of late-LTP by inhibition of the actin network during LTP induction.

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Activin increases the number of synaptic contacts and the length of dendritic spine necks by modulating spinal actin dynamics

Cited by 60 publications

References 48 publications

Canonical TGF-β Signaling Is Required for the Balance of Excitatory/Inhibitory Transmission within the Hippocampus and Prepulse Inhibition of Acoustic Startle

Canonical TGF-β Signaling Is Required for the Balance of Excitatory/Inhibitory Transmission within the Hippocampus and Prepulse Inhibition of Acoustic Startle

Involvement of the Serum Response Factor Coactivator Megakaryoblastic Leukemia (MKL) in the Activin-regulated Dendritic Complexity of Rat Cortical Neurons*

Interfering with the Actin Network and Its Effect on Long-Term Potentiation and Synaptic Tagging in Hippocampal CA1 Neurons in SlicesIn Vitro

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