AAV-Mediated Gene Delivery in a Feline Model of Sandhoff Disease Corrects Lysosomal Storage in the Central Nervous System

Rockwell, Hannah E.; McCurdy, Victoria J.; Eaton, Samuel C.; Wilson, Diane U.; Johnson, Aime K.; Randle, Ashley N.; Bradbury, Allison M.; Gray‐Edwards, Heather L.; Baker, Henry J.; Hudson, Judith A.; Cox, Nancy R.; Sena‐Esteves, Miguel; Seyfried, Thomas N.; Martin, Douglas R.

doi:10.1177/1759091415569908

Cited by 48 publications

(54 citation statements)

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“…Previous reports showed that all treated cats had clearly preserved neurologic function and improved disease phenotype, though mild symptoms such as fine tremors and slight hind limb weakness were present. Also, previously published postmortem analysis revealed above-normal levels of Hex activity throughout the brain and spinal cord, with clearance of GM2 ganglioside storage (McCurdy et al, 2015, Rockwell et al, 2015). Microglia from treated cats retained a ramified morphology and lacked expression of MHC-II in regions of cleared storage such as the thalamus (Fig.…”

Section: Resultsmentioning

confidence: 54%

“…Seven SD cats were treated with monocistronic AAVrh8 vectors encoding feline HEX α and β subunits between 4-7 weeks of age, prior to symptom onset. Two treatment cohorts were based on injection route: bilateral thalamic and DCN injection (n=3) (McCurdy et al, 2015) or bilateral thalamic and unilateral ICV injection (n=4) (Rockwell et al, 2015) (Table 1). Treated SD cats were euthanized 16 weeks after injection, an age comparable to the humane endpoint of untreated SD cats.…”

Section: Resultsmentioning

confidence: 99%

“…Treatment dramatically ameliorated clinical signs of disease, with cats demonstrating slight hind limb weakness and whole-body tremors that were mild (Thal+ICV) (Rockwell et al, 2015) or nonexistent (Thal+DCN) (McCurdy et al, 2015). The current report extends previous findings by showing that SD cats treated with AAV had marked attenuation of microglia activation, with a ramified morphology and lack of MHC-II expression, in areas of GM2 ganglioside clearance.…”

Section: Discussionmentioning

confidence: 99%

“…AAV vectors encoding feline α and β Hex subunits were injected bilaterally into the thalamus of SD cats, which reduced the immune response and increased survival to 10.4 ± 3.7 months of age, or > 2 times that of untreated cats (Bradbury et al, 2013). Further studies were conducted combining thalamic infusion with additional delivery routes such as bilateral injection into the deep cerebellar nuclei (DCN) (McCurdy et al, 2015), or intracerebroventricular (ICV) injection (Rockwell et al, 2015). Restoration of Hex activity, clearance of storage material, and a panel of biomarkers from combined delivery routes have been reported elsewhere (Bradbury et al, 2015, McCurdy et al, 2015, Rockwell et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

“…Further studies were conducted combining thalamic infusion with additional delivery routes such as bilateral injection into the deep cerebellar nuclei (DCN) (McCurdy et al, 2015), or intracerebroventricular (ICV) injection (Rockwell et al, 2015). Restoration of Hex activity, clearance of storage material, and a panel of biomarkers from combined delivery routes have been reported elsewhere (Bradbury et al, 2015, McCurdy et al, 2015, Rockwell et al, 2015). In the current study, we analyze the effect of intracranial gene therapy with thalamus + DCN and thalamus + ICV injection routes on the neuroinflammatory response in SD.…”

Section: Introductionmentioning

confidence: 99%

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AAV-mediated gene delivery attenuates neuroinflammation in feline Sandhoff disease

et al. 2017

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Sandhoff disease (SD) is a lysosomal storage disorder characterized by the absence of hydrolytic enzyme β-N-acetylhexosaminidase (Hex), which results in storage of GM2 ganglioside in neurons and unremitting neurodegeneration. Neuron loss initially affects fine motor skills, but rapidly progresses to loss of all body faculties, a vegetative state, and death by five years of age in humans. A well-established feline model of SD allows characterization of the disease in a large animal model and provides a means to test the safety and efficacy of therapeutic interventions before initiating clinical trials. In this study, we demonstrate a robust central nervous system (CNS) inflammatory response in feline SD, primarily marked by expansion and activation of the microglial cell population. Quantification of major histocompatibility complex II (MHC-II) labeling revealed significant up-regulation throughout the CNS with areas rich in white matter most severely affected. Expression of the leukocyte chemokine macrophage inflammatory protein-1 alpha (MIP-1α) was also up-regulated in the brain. SD cats were treated with intracranial delivery of adeno-associated viral (AAV) vectors expressing feline Hex, with a study endpoint 16 weeks post treatment. AAV-mediated gene delivery repressed the expansion and activation of microglia and normalized MHC-II and MIP-1α levels. These data reiterate the profound inflammatory response in SD and show that neuroinflammation is abrogated after AAV-mediated restoration of enzymatic activity.

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Section: Resultsmentioning

confidence: 54%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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AAV-mediated gene delivery attenuates neuroinflammation in feline Sandhoff disease

et al. 2017

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Imaging the Feline Neurologic System

Holmes¹

2020

Feline Diagnostic Imaging

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Abnormal epiphyseal development in a feline model of Sandhoff disease

McNulty

Prevatt

Nussbaum

et al. 2020

Journal Orthopaedic Research

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Sandhoff disease (SD) is caused by decreased function of the enzyme β‐N‐acetylhexosaminidase, resulting in accumulation of GM2 ganglioside in tissues. Neural tissue is primarily affected and individuals with the infantile form of the disease generally do not survive beyond 4 years of age. Current treatments address neurometabolic deficits to improve lifespan, however, this extended lifespan allows clinical disease to become manifest in other tissues, including the musculoskeletal system. The impact of SD on bone and joint tissues has yet to be fully determined. In a feline model of infantile SD, animals were treated by intracranial injection of adeno‐associated virus vectors to supply the central nervous system with corrective levels of hexosaminidase, resulting in a twofold to threefold increase in lifespan. As treated animals aged, signs of musculoskeletal disease were identified. The present study characterized bone and joint lesions from affected cats using micro‐computed tomography and histology. All affected cats had similar lesions, whether or not they were treated. SD cats displayed a significant reduction in metaphyseal trabecular bone and markedly abnormal size and shape of epiphyses. Abnormalities increased in severity with age and appear to be due to alteration in the function of chondrocytes within epiphyseal cartilage, particularly the articular‐epiphyseal complex. Older cats developed secondary osteoarthritic changes. The changes identified are similar to those seen in humans with mucopolysaccharidoses. Statement of clinical significance: the lesions identified will have significant implications on the quality of life of individuals whose lifespans are extended due to treatments for the primary neurological effects of SD.

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AAV-Mediated Gene Delivery in a Feline Model of Sandhoff Disease Corrects Lysosomal Storage in the Central Nervous System

Cited by 48 publications

References 46 publications

AAV-mediated gene delivery attenuates neuroinflammation in feline Sandhoff disease

AAV-mediated gene delivery attenuates neuroinflammation in feline Sandhoff disease

Imaging the Feline Neurologic System

Abnormal epiphyseal development in a feline model of Sandhoff disease

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