P1‐028: Overexpression of neprilysin reduces Abeta42‐induced neuron loss and intraneuronal Abeta42 deposits, but causes age‐dependent axon pathology in drosophila

Iijima-Ando, Kanae; Hearn, Stephen; Granger, Linda; Shenton, Christopher; Gatt, Anthony; Chiang, Hsueh‐Cheng; Hakker, Inessa; Zhong, Yi; Iijima, Koichi

doi:10.1016/j.jalz.2008.05.613

Cited by 3 publications

(4 citation statements)

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“…In addition to the effects on extracellular Aβ, NEP might modify AD-like pathology by reducing the accumulation of intracellular APP metabolites such as Aβ [22] , [23] . Increasingly, intracellular Aβ is being recognized as deleterious to the neuron as much or more than extracellular Aβ [23] , [24] , [25] .…”

Section: Resultsmentioning

confidence: 99%

“…A growing number of studies have shown that accumulation of intracellular Aβ could be deleterious[23], [24], [25], [42], [43] by triggering aberrant signaling via CREB[44]. Supporting this possibility, previous studies have shown that NEP ameliorates the deficits in the fly[22] and rodent models[23] by diminishing Aβ from the intracellular compartment. Although ApoBsecNEP was located in the soma and dendrites of neurons, it is not clear if the reduced intracellular Aβ may be driven by this source of NEP.…”

Section: Discussionmentioning

confidence: 95%

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Peripheral Delivery of a CNS Targeted, Metalo-Protease Reduces Aβ Toxicity in a Mouse Model of Alzheimer's Disease

et al. 2011

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Alzheimer's disease (AD), an incurable, progressive neurodegenerative disorder, is the most common form of dementia. Therapeutic options have been elusive due to the inability to deliver proteins across the blood-brain barrier (BBB). In order to improve the therapeutic potential for AD, we utilized a promising new approach for delivery of proteins across the BBB. We generated a lentivirus vector expressing the amyloid β-degrading enzyme, neprilysin, fused to the ApoB transport domain and delivered this by intra-peritoneal injection to amyloid protein precursor (APP) transgenic model of AD. Treated mice had reduced levels of Aβ, reduced plaques and increased synaptic density in the CNS. Furthermore, mice treated with the neprilysin targeting the CNS had a reversal of memory deficits. Thus, the addition of the ApoB transport domain to the secreted neprilysin generated a non-invasive therapeutic approach that may be a potential treatment in patients with AD.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 95%

Peripheral Delivery of a CNS Targeted, Metalo-Protease Reduces Aβ Toxicity in a Mouse Model of Alzheimer's Disease

et al. 2011

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“…Several studies have shown that intracellular A␤ could be deleterious (30, 35, 49 -51) by triggering an aberrant signaling via cAMP-response elementbinding protein (52). Supporting this possibility, previous studies have shown that neprilysin ameliorates the deficits in the fly (53) and rodent models (35) by diminishing A␤ from the intracellular compartment. Although ASN12 is primarily extracellular, it is not clear if this is capable of degrading A␤, and this shifts the equilibrium of A␤ from the intracellular space to the extracellular space, thus reducing the intracellular accumulation of A␤ indirectly.…”

Section: Discussionmentioning

confidence: 96%

A Neuroprotective Brain-penetrating Endopeptidase Fusion Protein Ameliorates Alzheimer Disease Pathology and Restores Neurogenesis

Spencer¹,

Verma

Desplats

et al. 2014

Journal of Biological Chemistry

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Background: Development of new therapeutic approaches for Alzheimer disease (AD) is crucial. Results: A recombinant enzyme engineered to cross the blood-brain barrier treats the accumulation of A␤ in a mouse model. Conclusion: This study shows a therapy can improve the symptoms of AD while also increasing the population of new neurons. Significance: The enzyme could be delivered weekly or even monthly to patients.

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“…Additional human AD pathologies feature learning and short-term memory (STM) loss, movement deficits, and early lethality. Each of these functional deficits is conserved in the AD-associated aged A42 model and has been previously documented and quantified (Iijima et al 2004;Iijima-Ando et al 2008;Wu et al 2019). Thus, we 7 asked whether these deficits occur during the early stages of A42-induced neuropathology and whether increasing Tip60 levels can protect against these deficits throughout neurodegenerative progression.…”

Section: Tip60 Hat Action Protects Against A42-induced Deficits In Lmentioning

confidence: 95%

Tip60 protects against amyloid-β peptide-induced transcriptomic alterations via different modes of action in early versus late stages of neurodegenerative progression

Zhang

Karisetty

Bhatnagar

et al. 2020

Preprint

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Alzheimer's disease is an age-related neurodegenerative disorder hallmarked by amyloid-β (Aβ) plaque accumulation, neuronal cell death, and cognitive deficits that worsen during disease progression. Histone acetylation dysregulation, caused by an imbalance between the histone acetyltransferases (HAT) Tip60 and histone deacetylase 2 (HDAC2), can directly contribute to AD pathology. Nevertheless, early and late-stage regulatory epigenetic alterations remain to be characterized. Here we profile Tip60 HAT/HDAC2 dynamics and transcriptional changes across early and late stage AD pathology in the Drosophila brain produced solely by human amyloid-β42.We show that early Aβ42 induction leads to disruption of Tip60 HAT/HDAC2 balance during early neurodegenerative stages preceding Aβ plaque accumulation that persists into late AD stages.Correlative transcriptome studies reveal alterations in biological processes we classified as transient (early-stage only), late-onset (late-stage only), and constant (both). Increasing Tip60 HAT levels in the Aβ42 fly brain protects against AD functional pathologies that include Aβ plaque accumulation, neural cell death, cognitive deficits, and shorter life-span. Strikingly, Tip60 also protects against Aβ42 induced transcriptomic alterations via distinct mechanisms during early and late stages of neurodegeneration. Our findings provide new insights into distinct modes of epigenetic gene alterations and Tip60 neuroprotection during early versus late stages in AD progression.

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P1‐028: Overexpression of neprilysin reduces Abeta42‐induced neuron loss and intraneuronal Abeta42 deposits, but causes age‐dependent axon pathology in drosophila

Cited by 3 publications

References 0 publications

Peripheral Delivery of a CNS Targeted, Metalo-Protease Reduces Aβ Toxicity in a Mouse Model of Alzheimer's Disease

Peripheral Delivery of a CNS Targeted, Metalo-Protease Reduces Aβ Toxicity in a Mouse Model of Alzheimer's Disease

A Neuroprotective Brain-penetrating Endopeptidase Fusion Protein Ameliorates Alzheimer Disease Pathology and Restores Neurogenesis

Tip60 protects against amyloid-β peptide-induced transcriptomic alterations via different modes of action in early versus late stages of neurodegenerative progression

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