Impaired Neurite Contact Guidance in Ubiquitin Ligase E3a (Ube3a)‐Deficient Hippocampal Neurons on Nanostructured Substrates

Tonazzini, Ilaria; Meucci, Sandro; Woerden, Geeske M. van; Elgersma, Ype; Cecchini, Marco

doi:10.1002/adhm.201500815

Cited by 18 publications

(27 citation statements)

References 82 publications

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“…Moreover, an overall excitatory network, due to a more severe decrease in inhibitory than excitatory inputs [197], possibly contributes to the increased seizure susceptibility observed in AS patients. In vitro studies using Ube3a knockdown or Ube3a KO neurons from mice have also shown that Ube3a loss of function decreased dendrite arborization, disrupted dendrite polarity and reduced apical dendrite length [198,199]. In addition, disrupted synaptic plasticity in the form of impaired LTP in different brain areas [45,193,200] and enhanced hippocampal mGluR-LTD [201] were also observed in AS mice (Table 1).…”

Section: Mtorc1 Signaling Pathway In Monogenic Autism Spectrum Dismentioning

confidence: 99%

Dysfunctional mTORC1 Signaling: A Convergent Mechanism between Syndromic and Nonsyndromic Forms of Autism Spectrum Disorder?

Magdalon

Sánchez-Sánchez

Griesi-Oliveira

et al. 2017

IJMS

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Whereas autism spectrum disorder (ASD) exhibits striking heterogeneity in genetics and clinical presentation, dysfunction of mechanistic target of rapamycin complex 1 (mTORC1) signaling pathway has been identified as a molecular feature common to several well-characterized syndromes with high prevalence of ASD. Additionally, recent findings have also implicated mTORC1 signaling abnormalities in a subset of nonsyndromic ASD, suggesting that defective mTORC1 pathway may be a potential converging mechanism in ASD pathology across different etiologies. However, the mechanistic evidence for a causal link between aberrant mTORC1 pathway activity and ASD neurobehavioral features varies depending on the ASD form involved. In this review, we first discuss six monogenic ASD-related syndromes, including both classical and potentially novel mTORopathies, highlighting their contribution to our understanding of the neurobiological mechanisms underlying ASD, and then we discuss existing evidence suggesting that aberrant mTORC1 signaling may also play a role in nonsyndromic ASD.

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Section: Mtorc1 Signaling Pathway In Monogenic Autism Spectrum Dismentioning

confidence: 99%

Dysfunctional mTORC1 Signaling: A Convergent Mechanism between Syndromic and Nonsyndromic Forms of Autism Spectrum Disorder?

Magdalon

Sánchez-Sánchez

Griesi-Oliveira

et al. 2017

IJMS

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“…Because we know that neurite growth is usually favored along NGs (i.e. aligned neurites are longer than misaligned ones) 55 , we quantitatively examined the spatial development of neurite arborization and we calculated the total length of the neurites aligned (alignment angle 0-15°) or perpendicular (alignment angle 75°-90°) to NG pattern on each substrate (reported in % over the total network length analyzed) (Fig. 8b).…”

Section: Scientific Reports |mentioning

confidence: 99%

“…Cell lysates (10 µg/line) were processed by immunoblot, as in 55 . Briefly, samples were resolved by gel electrophoresis (SDS-PAGE) using Gel Criterion XT-Precasted polyacrylamide gel 4-12% Bis-Tris (Biorad), transferred to nitrocellulose membranes by Trans-Blot Turbo transfer system (Biorad) and probed overnight at 4 °C with primary antibodies.…”

Section: Focal Adhesion Experiments and Live Cell Total Internal Reflmentioning

confidence: 99%

“…YAP immunocytochemistry and fluorescence confocal microscopy. PC12 cells were cultured, fixed for 15 min with 4% formaldehyde with 4% sucrose in PBS at room temperature and processed as previously reported 55 . Here cells were incubated with primary anti-YAP1 antibody (1:500, ab39361) and phalloidin-Alexa fluor 647 (1:40, Thermo Fisher A22287) in GDB buffer (0.2% BSA, 0.8 M NaCl, 0.5% Triton X-100, 30 mM phosphate buffer, pH 7.4) overnight at 4 °C and then with appropriate secondary antibody conjugated to AlexaFluor 488; in the end samples were mounted using Fluorashield mounting medium with 4′,6-diamidin-2-fenilindolo (DAPI) to stain nuclei (Sigma, F6057).…”

Section: Focal Adhesion Experiments and Live Cell Total Internal Reflmentioning

confidence: 99%

“…primary hippocampal neurons. Hippocampal neuronal cultures (HNs) were prepared from brains of single E17-18 mouse embryos (C57 background), as previously described 55 . Mice were maintained under standard housing conditions and used according to the protocols and ethical guidelines approved by the Italian Ministry of Health (Permit Number: CBS-not.…”

Section: Focal Adhesion Experiments and Live Cell Total Internal Reflmentioning

confidence: 99%

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Neuronal contact guidance and YAP signaling on ultra-small nanogratings

Tonazzini

Masciullo

Savi

et al. 2020

Sci Rep

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contact interaction of neuronal cells with extracellular nanometric features can be exploited to investigate and modulate cellular responses. By exploiting nanogratings (nGs) with linewidth from 500 nm down to 100 nm, we here study neurite contact guidance along ultra-small directional topographies. the impact of nG lateral dimension on the neuronal morphotype, neurite alignment, focal adhesion (fA) development and YAp activation is investigated in nerve growth factor (nGf)differentiating PC12 cells and in primary hippocampal neurons, by confocal and live-cell total internal reflection fluorescence (TIRF) microscopy, and at molecular level. We demonstrate that loss of neurite guidance occurs in NGs with periodicity below 400 nm and correlates with a loss of FA lateral constriction and spatial organization. We found that YAP intracellular localization is modulated by the presence of nGs, but it is not sensitive to their periodicity. nocodazole, a drug that can increase cell contractility, is finally tested for rescuing neurite alignment showing mild ameliorative effects. Our results provide new indications for a rational design of biocompatible scaffolds for enhancing nerveregeneration processes.With its chemical and physical complexity, the extracellular environment can drive cell morphogenesis, migration and differentiation 1-4 , In particular, the contact interaction of cells with extracellular nanometric features has a primary role in regulating many physiological 5-12 and pathological processes 13 in vivo, and can be exploited to modulate cell responses in vitro [14][15][16][17] . Cells gather morphological information about the Extracellular matrix (ECM) through integrin-mediated adhesion clusters, called the focal adhesions (FAs), which act as topographical sensors. FAs can integrate multiple nanotopographical details into specific biomolecular instructions via the cytoskeletal signaling, which lastly regulates cell contractility, morphology and migration 9,18,19 , Artificial scaffolds with controlled micro/nano-topographies are definitively the apparatus of choice to better understand the response mechanisms of cells to external stimuli. They indeed allow to select and finely tune specific topographical aspects and selectively study their interaction with living system in vitro. The scientific literature reports many examples of nanostructures that can, for example, direct stem cell fate 20-22 , neuronal and glial adhesion 23-25 , differentiation 26 , polarization, and neurite orientation 14,18 , Our previous studies have demonstrated that plastic nanogratings (NGs) (i.e. alternating lines of sub-micron grooves and ridges, in the range between 500 and 2000 nm in linewidth) can promote neurite alignment and bipolarity of PC12 neuronal cells upon administration of nerve grow factor (NGF), simply by the contact guidance mechanism 27,28 , In these studies, adhesion on the ridges imposes a geometrical and directional constraint to FAs that results in neuronal polarization via the ROCK-mediated pathway 14,29-31 ...

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Interactions of Neurons with Physical Environments

Marcus

Baranes

Park

et al. 2017

Adv Healthcare Materials

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Nerve growth strongly relies on multiple chemical and physical signals throughout development and regeneration. Currently, a cure for injured neuronal tissue is an unmet need. Recent advances in fabrication technologies and materials led to the development of synthetic interfaces for neurons. Such engineered platforms that come in 2D and 3D forms can mimic the native extracellular environment and create a deeper understanding of neuronal growth mechanisms, and ultimately advance the development of potential therapies for neuronal regeneration. This progress report aims to present a comprehensive discussion of this field, focusing on physical feature design and fabrication with additional information about considerations of chemical modifications. We review studies of platforms generated with a range of topographies, from micro-scale features down to topographical elements at the nanoscale that demonstrate effective interactions with neuronal cells. Fabrication methods are discussed as well as their biological outcomes. This report highlights the interplay between neuronal systems and the important roles played by topography on neuronal differentiation, outgrowth, and development. The influence of substrate structures on different neuronal cells and parameters including cell fate, outgrowth, intracellular remodeling, gene expression and activity is discussed. Matching these effects to specific needs may lead to the emergence of clinical solutions for patients suffering from neuronal injuries or brain-machine interface (BMI) applications.

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Impaired Neurite Contact Guidance in Ubiquitin Ligase E3a (Ube3a)‐Deficient Hippocampal Neurons on Nanostructured Substrates

Cited by 18 publications

References 82 publications

Dysfunctional mTORC1 Signaling: A Convergent Mechanism between Syndromic and Nonsyndromic Forms of Autism Spectrum Disorder?

Dysfunctional mTORC1 Signaling: A Convergent Mechanism between Syndromic and Nonsyndromic Forms of Autism Spectrum Disorder?

Neuronal contact guidance and YAP signaling on ultra-small nanogratings

Interactions of Neurons with Physical Environments

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