Caspase-2 is required for dendritic spine and behavioural alterations in J20 APP transgenic mice

Pozueta, Julio; Lefort, Roger; Ribé, Elena M.; Troy, Carol M.; Arancio, Ottavio; Shelanski, Michael L.

doi:10.1038/ncomms2927

Cited by 89 publications

(109 citation statements)

References 57 publications

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“…At 12-18 months of age, these mice have also been reported to have significantly increased RhoA levels and decreased Rac1 levels in the brain [31]. Our recent studies in the hAPP J20 (Swedish and Indiana mutations) AD mouse model show a strong correlation between dendritic spine loss and behavioral deficits with a significant increase in RhoA activity [32]. In vitro studies in cultured cells also reflect these changes.…”

Section: Rho-guanosine Triphosphatases At the Center Of Ad Pathologymentioning

confidence: 65%

“…In vitro studies in cultured cells also reflect these changes. Aβ oligomers trigger a significant increase in RhoA activity in both SY5Y cells and in cultured hippocampal neurons [31][32][33][34]. Cdc42 and Rac1 levels have been reported to be elevated in select neuronal populations in AD brains compared with age-matched controls and have been proposed to perhaps play a role in activating cell cycle-related genes [35].…”

Section: Rho-guanosine Triphosphatases At the Center Of Ad Pathologymentioning

confidence: 99%

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Reversing Synapse Loss in Alzheimer's Disease: Rho-Guanosine Triphosphatases and Insights from Other Brain Disorders

Lefort

2015

Neurotherapeutics

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Alzheimer's disease (AD) is a monumental public health crisis with no effective cure or treatment. To date, therapeutic strategies have focused almost exclusively on upstream signaling events in the disease, namely on β-amyloid and amyloid precursor protein processing, and have, unfortunately, yielded few, if any, promising results. An alternative approach may be to target signaling events downstream of β-amyloid and even tau. However, with so many pathways already linked to the disease, understanding which ones are "drivers" versus "passengers" in the pathogenesis of the disease remains a tremendous challenge. Given the critical roles of Rho-guanosine triphosphatases (GTPases) in regulating the actin cytoskeleton and spine dynamics, and the strong association between spine abnormalities and cognition, it is not surprising that mutations in a number of genes involved in RhoGTPase signaling have been implicated in several brain disorders, including schizophrenia and autism. And now, there is mounting literature implicating Rho-GTPase signaling in AD pathogenesis as well. Here, I review this evidence, with a particular emphasis on the regulators of Rho-GTPase signaling, namely guanine nucleotide exchange factors and GTPaseactivating proteins. Several of these have been linked to various aspects of AD, and each offers a novel potential therapeutic target for AD.

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Section: Rho-guanosine Triphosphatases At the Center Of Ad Pathologymentioning

confidence: 65%

Section: Rho-guanosine Triphosphatases At the Center Of Ad Pathologymentioning

confidence: 99%

Reversing Synapse Loss in Alzheimer's Disease: Rho-Guanosine Triphosphatases and Insights from Other Brain Disorders

Lefort

2015

Neurotherapeutics

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“…This was attributed to an important role for caspse-2 in controlling dendrite spine density. 200 Caspase-2 was found to activate the RhoA/ROCK-II signaling pathway, leading to collapse of dendritic spines.…”

Section: Caspases In Neural Developmentmentioning

confidence: 99%

Old, new and emerging functions of caspases

et al. 2014

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Caspases are proteases with a well-defined role in apoptosis. However, increasing evidence indicates multiple functions of caspases outside apoptosis. Caspase-1 and caspase-11 have roles in inflammation and mediating inflammatory cell death by pyroptosis. Similarly, caspase-8 has dual role in cell death, mediating both receptor-mediated apoptosis and in its absence, necroptosis. Caspase-8 also functions in maintenance and homeostasis of the adult T-cell population. Caspase-3 has important roles in tissue differentiation, regeneration and neural development in ways that are distinct and do not involve any apoptotic activity. Several other caspases have demonstrated anti-tumor roles. Notable among them are caspase-2, -8 and -14. However, increased caspase-2 and -8 expression in certain types of tumor has also been linked to promoting tumorigenesis. Increased levels of caspase-3 in tumor cells causes apoptosis and secretion of paracrine factors that promotes compensatory proliferation in surrounding normal tissues, tumor cell repopulation and presents a barrier for effective therapeutic strategies. Besides this caspase-2 has emerged as a unique caspase with potential roles in maintaining genomic stability, metabolism, autophagy and aging. The present review focuses on some of these less studied and emerging functions of mammalian caspases.

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“…Deregulation of Rho GTPase signaling has been implicated in neurotoxicity by Ab (Chacon et al, 2011;Petratos et al, 2008;Pozueta et al, 2013). Alterations in actin dynamics is generally considered the mechanism by which Rho contributes to the collapse of dendritic spines and impairs synaptic transmission, all early events occurring in neurons exposed to Ab (Lambert et al, 1998;Lefort et al, 2012;Lesné et al, 2006;Nimmrich and Ebert, 2009;Shankar et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

“…However, it is not known whether neurotoxicity might also derive from changes in MT dynamics and/or MT post-translational modifications induced by Rho activation through the action on its effector mDia1 (Goulimari et al, 2005;Palazzo et al, 2001a). In neurons, APP and caspase-2 can regulate RhoA activation, and cells lacking either APP or caspase-2 are completely immune to Ab synaptotoxicity (Pozueta et al, 2013;Troy et al, 2000). In addition, dimerization of cellsurface APP by cross-linking cell-surface APP with a divalent antibody is sufficient to mimic the toxic effects of Ab in neurons (Lefort et al, 2012;Rohn et al, 2000).…”

Section: Introductionmentioning

confidence: 99%

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

Pianu

Lefort

Thuiliere

et al. 2014

Journal of Cell Science

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Interference with microtubule stability by beta-amyloid peptide (Ab) has been shown to disrupt dendritic function and axonal trafficking, both early events in Alzheimer's disease. However, it is unclear whether Ab regulation of microtubule dynamics can occur independently of its action on tau. RhoA has been implicated in neurotoxicity by Ab but the mechanism by which this activation generates cytoskeletal changes is also unclear. We found that oligomeric Ab 1-42 induced the formation of stable detyrosinated microtubules in NIH3T3 cells and this function resulted from the activation of a RhoA-dependent microtubule stabilization pathway regulated by integrin signaling and the formin mDia1. Induction of microtubule stability by Ab was also initiated by dimerization of APP and required caspase activity, two previously characterized regulators of neurotoxicity downstream of Ab. Finally, we found that this function was conserved in primary neurons and abolished by Rho inactivation, reinforcing a link between induction of stable detyrosinated microtubules and neuropathogenesis by Ab. Our study reveals a novel activity of Ab on the microtubule cytoskeleton that is independent of tau and associated with pathways linked to microtubule stabilization and Ab-mediated neurotoxicity.

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Caspase-2 is required for dendritic spine and behavioural alterations in J20 APP transgenic mice

Cited by 89 publications

References 57 publications

Reversing Synapse Loss in Alzheimer's Disease: Rho-Guanosine Triphosphatases and Insights from Other Brain Disorders

Reversing Synapse Loss in Alzheimer's Disease: Rho-Guanosine Triphosphatases and Insights from Other Brain Disorders

Old, new and emerging functions of caspases

Amyloid beta1-42 peptide regulates microtubule stability independently of tau

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