Docosahexaenoic Acid Protects from Dendritic Pathology in an Alzheimer's Disease Mouse Model

Calon, Frédéric; Lim, Giselle P.; Yang, Fusheng; Morita, Takashi; Teter, Bruce; Ubeda, Oliver J.; Rostaing, Phillippe; Triller, Antoine; Salem, Norman; Ashe, Karen H.; Frautschy, Sally A.; Cole, Greg M.

doi:10.1016/j.neuron.2004.08.013

Cited by 661 publications

(549 citation statements)

References 83 publications

(144 reference statements)

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“…DHA depletion aggravated cognitive deficits in the Morris Water Maze in the Tg2576 mouse, while DHA supplementation was protective [7] and reduced amyloid, even late in life [14]. Anti-amyloid activities include modulation of secretase activities via membrane "fluidity"/protein mobility changes or Akt > GSK regulation of ␥-secretase [25] and induction of anti-amyloidogenic transthyretin [26].…”

Section: Omega-3 Fatty Acidsmentioning

confidence: 99%

“…Aged Tg2576 APPsw transgene-positive mice placed from 17 to 22 months on a safflower oil rich, DHA-depleting diet exhibited increased oxidative damage and transgenedependent loss of CNS DHA and massive (70-95%) loss of postsynaptic proteins like the actin-regulatory drebrin, a dendritic spine protein known to be 70-90% lost in AD [7,27] and NR2b [6]. Greater depletion of DHA in Tg2576 may be driven by A␤ aggregates causing DHA oxidation.…”

Section: Omega-3 Fatty Acidsmentioning

confidence: 99%

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Prevention of Alzheimer's disease: Omega-3 fatty acid and phenolic anti-oxidant interventions

Cole

Lim

Yang

et al. 2005

Neurobiology of Aging

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197

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Alzheimer's disease (AD) and cardiovascular disease (CVD) are syndromes of aging that share analogous lesions and risk factors, involving lipoproteins, oxidative damage and inflammation. Unlike in CVD, in AD, sensitive biomarkers are unknown, and high-risk groups are understudied. To identify potential prevention strategies in AD, we have focused on pre-clinical models (transgenic and amyloid infusion models), testing dietary/lifestyle factors strongly implicated in reducing risk in epidemiological studies. Initially, we reported the impact of non-steroidal anti-inflammatory drugs (NSAIDs), notably ibuprofen, which reduced amyloid accumulation, but suppressed few inflammatory markers and without reducing oxidative damage. Safety concerns with chronic NSAIDs led to a screen of alternative NSAIDs and identification of the phenolic anti-inflammatory/anti-oxidant compound curcumin, the yellow pigment in turmeric that we found targeted multiple AD pathogenic cascades. The dietary omega-3 fatty acid, docosahexaenoic acid (DHA), also limited amyloid, oxidative damage and synaptic and cognitive deficits in a transgenic mouse model. Both DHA and curcumin have favorable safety profiles, epidemiology and efficacy, and may exert general anti-aging benefits (anti-cancer and cardioprotective.)

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Section: Omega-3 Fatty Acidsmentioning

confidence: 99%

Section: Omega-3 Fatty Acidsmentioning

confidence: 99%

Prevention of Alzheimer's disease: Omega-3 fatty acid and phenolic anti-oxidant interventions

Cole

Lim

Yang

et al. 2005

Neurobiology of Aging

Self Cite

197

117

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“…This occurs in mild cognitive impairment (Counts et al, 2012), Alzheimer's disease (Harigaya et al, 1996;Hatanpaa et al, 1999;Shim and Lubec, 2002;Calon et al, 2004;Zhao et al, 2006) and Down's syndrome, where individuals inevitably develop Alzheimer's (Weitzdoerfer et al, 2001;Shim and Lubec, 2002). Whether or not drebrin loss from dendritic spines is causal to cognitive decline in Alzheimer's disease and related cognitive disorders is not fully resolved.…”

Section: Drebrin Loss From Dendritic Spines Precedes Synapse Lossmentioning

confidence: 99%

“…Transgenic mouse models of familial Alzheimer's disease also show a loss of drebrin from dendritic spines (Lee and Aoki 2012;Calon et al, 2004;Calon et al, 2005;Mahadomrongkul et al, 2005;Aoki et al, 2007;Lacor et al, 2007). Drebrin loss occurs before loss of pre-synaptic markers, such as synaptophysin, suggesting it precedes synapse loss (Counts et al, 2012).…”

Section: Drebrin Loss From Dendritic Spines Precedes Synapse Lossmentioning

confidence: 99%

“…Although proteolysis at synapses increases in Alzheimer's disease, drebrin breakdown products have not been seen. Proteolytic fragments might have been missed because only one antibody had been used previously to detect drebrin by immunoblotting in Alzheimer's disease brain tissue and transgenic mouse models of Alzheimer's disease and the epitope that it recognises, which is in the C-terminal BB, might be lost from proteolytic fragments (Hatanpaa et al, 1999;Calon et al, 2004;Zhao et al, 2006;Counts et al 2012). It is unclear whether the loss of drebrin through proteolysis causes a loss of drebrin function or a dominant negative effect through one of the proteolytic fragments.…”

Section: Drebrin Loss From Dendritic Spines Precedes Synapse Lossmentioning

confidence: 99%

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The role of the drebrin/EB3/Cdk5 pathway in dendritic spine plasticity, implications for Alzheimer’s disease

Gordon‐Weeks

2016

Brain Research Bulletin

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3 Highlights The cytoskeleton underlies cell shape changes in response to guidance cues  The drebrin/EB3/Cdk5 pathway couples dynamic microtubules to actin filaments  Microtubule insertion into dendritic spines facilitates spine plasticity  Microtubule insertion into dendritic spines requires drebrin and EB3  Loss of drebrin contributes to cognitive decline In Alzheimer's disease AbstractThe drebrin/EB3/Cdk5 intracellular signaling pathway couples actin filaments to dynamic microtubules in cellular settings where cells are changing shape. The pathway has been most intensively studied in neuronal development, particularly neuritogenesis and neuronal migration, and in synaptic plasticity at dendritic spines in mature neurons. Drebrin is an actin filament sidebinding and bundling protein that stabilizes actin filaments. The end-binding (EB) proteins are microtubule plus-end tracking proteins (+TIPs) that localize to the growing plus-ends of dynamic microtubules and regulate their behavior and the binding of other +TIP proteins. EB3 binds specifically to drebrin when drebrin is bound to actin filaments, for example at the base of a growth cone filopodium, and EB3 is located at the plus-end of a growing microtubule inserting into the filopodium. This interaction therefore forms the basis for coupling dynamic microtubules to actin filaments in growth cones of developing neurons. Appropriate responses to growth cone guidance cues depend on actin filament/microtubule co-ordination in the growth cone, although the role of the drebrin/EB3/Cdk5 pathway in this context has not been directly tested. A similar cytoskeleton coupling pathway operates in dendritic spines in mature neurons where the activity-dependent insertion of dynamic microtubules into dendritic spines is facilitated by drebrin binding to EB3.Microtubule insertion into dendritic spines drives spine maturation during long-term potentiation and therefore has a role in synaptic plasticity and memory formation. In Alzheimer's disease and related chronic neurodegenerative diseases, there is an early and dramatic loss of drebrin from dendritic spines that precedes synapse loss and neurodegeneration and might contribute to a failure of synaptic plasticity and hence to cognitive decline.4

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Fish Consumption and Cognitive Decline With Age in a Large Community Study

Morris¹,

Evans²,

Tangney³

et al. 2005

Arch Neurol

363

180

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Docosahexaenoic Acid Protects from Dendritic Pathology in an Alzheimer's Disease Mouse Model

Cited by 661 publications

References 83 publications

Prevention of Alzheimer's disease: Omega-3 fatty acid and phenolic anti-oxidant interventions

Prevention of Alzheimer's disease: Omega-3 fatty acid and phenolic anti-oxidant interventions

The role of the drebrin/EB3/Cdk5 pathway in dendritic spine plasticity, implications for Alzheimer’s disease

Fish Consumption and Cognitive Decline With Age in a Large Community Study

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