AAVrh.10-Mediated APOE2 Central Nervous System Gene Therapy for APOE4-Associated Alzheimer's Disease

Rosenberg, Jonathan B.; Kaplitt, Michael G.; De, Bishnu P.; Chen, Alvin; Flagiello, Thomas; Salami, Christiana O; Pey, Eduard; Zhao, Lingzhi; Arbona, Rodolfo J Ricart; Monette, Sébastien; Dyke, Jonathan P.; Ballon, Douglas; Kaminsky, Stephen M.; Sondhi, Dolan; Petsko, Gregory A.; Paul, Steven M.; Crystal, Ronald G.

doi:10.1089/humc.2017.231

Cited by 109 publications

(70 citation statements)

References 99 publications

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“…Intrathecal delivery, direct spinal cord, and brain injections have all demonstrated safety. Presently, there are several viral-mediated gene-therapy clinical trials for neurodegenerative diseases (3), and recent intracisternal AAV delivery in nonhuman primates demonstrated wide transgene expression (35). In December 2017, the Food and Drug Administration approved the first-ever AAV-mediated gene therapy for retinal dystrophy, demonstrating a monumental shift in CNS therapies.…”

Section: Discussionmentioning

confidence: 99%

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice

et al. 2019

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Interventions that preserve motor neurons or restore functional motor neuroplasticity may extend longevity in amyotrophic lateral sclerosis (ALS). Delivery of neurotrophins may potentially revive degenerating motor neurons, yet this approach is dependent on the proper subcellular localization of neurotrophin receptor (NTR) to plasmalemmal signaling microdomains, termed membrane/lipid rafts (MLRs). We previously showed that over‐expression of synapsin‐driven caveolin‐1 (Cav‐1) (SynCav1) increases MLR localization of NTR [e.g., receptor tyrosine kinase B (TrkB)], promotes hippocampal synaptic and neuroplasticity, and significantly improves learning and memory in aged mice. The present study crossed a SynCav1 transgene‐positive (SynCav1+) mouse with the mutant human superoxide dismutase glycine to alanine point mutation at amino acid 93 (hSOD1G93A) mouse model of ALS. When compared with hSOD1G93A, hSOD1G93A/SynCav1+ mice exhibited greater body weight and longer survival as well as better motor function. Microscopic analyses of hSOD1G93A/SynCav1+ spinal cords revealed preserved spinal cord α‐motor neurons and preserved mitochondrial morphology. Moreover, hSOD1G93A/SynCav1+ spinal cords contained more MLRs (cholera toxin subunit B positive) and MLR‐associated TrkB and Cav‐1 protein expression. These findings demonstrate that SynCav1 delays disease progression in a mouse model of ALS, potentially by preserving or restoring NTR expression and localization to MLRs.—Sawada, A., Wang, S., Jian, M., Leem, J., Wackerbarth, J., Egawa, J., Schilling, J. M., Platoshyn, O., Zemljic‐Harpf, A., Roth, D. M., Patel, H. H., Patel, P. M., Marsala, M., Head, B. P. Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1G93A mice. FASEB J. 33, 7545–7554 (2019). http://www.fasebj.org

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Section: Discussionmentioning

confidence: 99%

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice

et al. 2019

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“…This study also showed that gene delivery of APOE2 was most effective before the onset of amyloid burden, suggesting that in order to be a successful therapy the AAV would need to be injected much before the onset of symptoms in patients which poses its own challenges. Further translational studies on non-human primates revealed that intra-cisternal delivery of AAV-APOE2 led to widespread expression in the CNS which established a safe procedure for CNS delivery of biologics [166]. Because of the inherent risk in any surgical procedure inside the CNS, whether such AAV-APOE2 biologics can be directly delivered into the AD-affected areas of the human CNS needs to be cautiously determined.…”

Section: Aav-apoe2 Biologic Therapymentioning

confidence: 99%

Therapeutic approaches targeting Apolipoprotein E function in Alzheimer’s disease

Williams

Borchelt

Chakrabarty

2020

Mol Neurodegeneration

111

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One of the primary genetic risk factors for Alzheimer's disease (AD) is the presence of the Ɛ4 allele of apolipoprotein E (APOE). APOE is a polymorphic lipoprotein that is a major cholesterol carrier in the brain. It is also involved in various cellular functions such as neuronal signaling, neuroinflammation and glucose metabolism. Humans predominantly possess three different allelic variants of APOE, termed E2, E3, and E4, with the E3 allele being the most common. The presence of the E4 allele is associated with increased risk of AD whereas E2 reduces the risk. To understand the molecular mechanisms that underlie APOE-related genetic risk, considerable effort has been devoted towards developing cellular and animal models. Data from these models indicate that APOE4 exacerbates amyloid β plaque burden in a dose-dependent manner. and may also enhance tau pathogenesis in an isoform-dependent manner. Other studies have suggested APOE4 increases the risk of AD by mechanisms that are distinct from modulation of Aβ or tau pathology. Further, whether plasma APOE, by influencing systemic metabolic pathways, can also possibly alter CNS function indirectly is not complete;y understood. Collectively, the available studies suggest that APOE may impact multiple signaling pathways and thus investigators have sought therapeutics that would disrupt pathological functions of APOE while preserving or enhancing beneficial functions. This review will highlight some of the therapeutic strategies that are currently being pursued to target APOE4 towards preventing or treating AD and we will discuss additional strategies that holds promise for the future.

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“…AAVrh.10CisTau coding for the anti-Tau monoclonal Cis-Tau 33,59 ; and AAVrh.10Null used as a control, identical to the other vectors but with no gene coding sequence. 41 PHF1 hybridoma cell cDNA (gift from Peter Davies, Albert Einstein College of Medicine) was amplified and synthesized in two independent reactions using primer annealing conserved regions of the constant heavy and light chains. The cDNA containing the mouse heavy chain sequence from IgG1 and the mouse Kappa light chain sequence was amplified using nested primers, cloned into a TOPO vector (Thermo Fisher Scientific, Inc., Carlsbad, CA) and sequenced.…”

Section: Aavrh10 Vectorsmentioning

confidence: 99%

“…All vectors were produced using 293T cells as described previously. [40][41][42][43]60 Briefly, the expression plasmid and the AAVrh.10 packaging-Ad helper hybrid plasmid pPAK-MArh.10 were cotransfected into 293T cells using the PEI transfection reagent (Polysciences, Warrington, PA). At 72 h post-transfection, cells were harvested and lysate prepared using five cycles of freeze/thaw.…”

Section: Aavrh10 Vectorsmentioning

confidence: 99%

“…To test this hypothesis, we used an AAVrh.10 serotype gene transfer vector because there is low anti-AAVrh.10 seroprevalence in humans, 39 AAVrh.10 mediates high expression of transgenes in neurons in experimental animal models, [40][41][42][43] and AAVrh.10 vectors have been used safely in clinical trials to deliver the therapeutic genes to the CNS of children with mucopolysaccharidosis IIIB and metachromatic leukodystrophy. 44,45 To evaluate an AAVrh.10 anti-Tau-based therapy, we developed a murine repetitive TBI model that is mechanistically unlike the age-related degenerative disease models.…”

Section: Introductionmentioning

confidence: 99%

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Anti-Phospho-Tau Gene Therapy for Chronic Traumatic Encephalopathy

et al. 2020

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Chronic traumatic encephalopathy (CTE) is a progressive neurodegenerative disorder caused by repetitive trauma to the central nervous system (CNS) suffered by soldiers, contact sport athletes, and civilians following accident-related trauma. CTE is a CNS tauopathy, with trauma-induced inflammation leading to accumulation of hyperphosphorylated forms of the microtubule-binding protein Tau (pTau), resulting in neurofibrillary tangles and progressive loss of neurons. At present, there are no therapies to treat CTE. We hypothesized that direct CNS administration of an adeno-associated virus (AAV) vector coding for an anti-pTau antibody would generate sufficient levels of anti-pTau in the CNS to suppress pTau accumulation thus interrupting the pathogenic process. Using a serotype AAVrh.10 gene transfer vector coding for a monoclonal antibody directed against pTau, we demonstrate the feasibility of this strategy in a murine CTE model in which pTau accumulation was elicited by repeated traumatic brain injury (TBI) using a closed cortical impact procedure over 5 days. Direct delivery of AAVrh.10 expression vectors coding for either of the two different anti-pTau antibodies to the hippocampus of these TBI mice significantly reduced pTau levels across the CNS. Using doses that can be safely scaled to humans, the data demonstrate that CNS administration of AAVrh.10anti-pTau is effective, providing a new strategy to interrupt the CTE consequences of TBI.

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AAVrh.10-Mediated APOE2 Central Nervous System Gene Therapy for APOE4-Associated Alzheimer's Disease

Cited by 109 publications

References 99 publications

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice

Therapeutic approaches targeting Apolipoprotein E function in Alzheimer’s disease

Anti-Phospho-Tau Gene Therapy for Chronic Traumatic Encephalopathy

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AAVrh.10-Mediated APOE2 Central Nervous System Gene Therapy for APOE4-Associated Alzheimer's Disease

Cited by 109 publications

References 99 publications

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 G93A mice

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 G93A mice

Therapeutic approaches targeting Apolipoprotein E function in Alzheimer’s disease

Anti-Phospho-Tau Gene Therapy for Chronic Traumatic Encephalopathy

Contact Info

Product

Resources

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Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice

Neuron‐targeted caveolin‐1 improves neuromuscular function and extends survival in SOD1 ^G93A mice