Morphological and Behavioral Impact of AAV2/5-Mediated Overexpression of Human Wildtype Alpha-Synuclein in the Rat Nigrostriatal System

Gombash, Sara E.; Manfredsson, Fredric P.; Kemp, Christopher J.; Kuhn, Nathan C.; Fleming, Sheila M.; Egan, Ann E.; Grant, Laura M.; Ciucci, Michelle R.; MacKeigan, Jeffrey P.; Sortwell, Caryl E.

doi:10.1371/journal.pone.0081426

Cited by 75 publications

(94 citation statements)

References 57 publications

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“…We first verified, as demonstrated previously, that our rAAV2/5 expressing GFP is not toxic to nigral dopaminergic neurons of the SNpc (Gombash et al , 2013). Age-related reductions in total nigral dopaminergic neurons are not a factor in our present results as equivalent numbers of nigral THir neurons are present in the SD rat at 20 months as compared to 3 months of age.…”

Section: Discussionsupporting

confidence: 68%

“…Particles were purified using iodixanol gradients and Q-sepharose chromatography, and dotblot was used to determine vector titer (Zolotukhin et al , 1999). The vector titer used in this study was 5.88 × 10 13 genomes/mL (Gombash et al , 2013). In order to preserve the viral stability and titer, viral preparations were stored at 4°C and never frozen.…”

Section: Methodsmentioning

confidence: 99%

“…Rats were placed in a stereotaxic frame and two 2μL injections of rAAV2/5 were injected in the left SN at coordinates (from dura) AP −5.3mm, ML +2.0mm, DV −7.2mm, and AP −6.0mm, ML +2.0mm, and DV −7.2mm as previously described (Gombash et al , 2013). A Hamilton syringe fitted with a glass capillary needle (Hamilton Gas Tight syringe 80,000, 26s/2” needle; Hamilton, Reno, NV; coated in SigmaCote) was used for injection.…”

Section: Methodsmentioning

confidence: 99%

“…The present study sought to determine whether viral vector-mediated transgene expression was reduced in the aged rat nigrostriatal system as compared to the young adult. We utilized the rAAV2/5 serotype to examine this question because of its efficient transduction of nigral neurons (Burger et al , 2004; Gombash et al , 2013). Intranigral injections of rAAV serotype 2/5 expressing green fluorescent protein (rAAV2/5 GFP) resulted in significantly reduced exogenous protein expression in the aged rat brain as compared to the young adult brain.…”

Section: Introductionmentioning

confidence: 99%

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Recombinant adenoassociated virus 2/5-mediated gene transfer is reduced in the aged rat midbrain

Polinski

Gombash

Manfredsson

et al. 2015

Neurobiology of Aging

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Clinical trials are examining the efficacy of viral vector-mediated gene delivery for treating Parkinson’s disease (PD). While viral vector strategies have been successful in preclinical studies, to date clinical trials have disappointed. This may be due to the fact that preclinical studies fail to account for aging. Aging is the single greatest risk factor for developing PD and age alters cellular processes utilized by viral vectors. We hypothesized that the aged brain would be relatively resistant to transduction when compared to the young adult. We examined recombinant adeno-associated virus 2/5 mediated green fluorescent protein (rAAV2/5 GFP) expression in the young adult and aged rat nigrostriatal system. GFP overexpression was produced in both age groups. However, following rAAV2/5 GFP injection to the substantia nigra (SN) aged rats displayed 40-60% less GFP protein in the striatum, regardless of rat strain or duration of expression. Further, aged rats exhibited 40% fewer cells expressing GFP and 4-fold less GFP mRNA. rAAV2/5-mediated gene transfer is compromised in the aged rat midbrain, with deficiencies in early steps of transduction leading to significantly less mRNA and protein expression.

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Section: Discussionsupporting

confidence: 68%

Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Recombinant adenoassociated virus 2/5-mediated gene transfer is reduced in the aged rat midbrain

Polinski

Gombash

Manfredsson

et al. 2015

Neurobiology of Aging

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“…Similar to toxin models, viral vectors overexpressing aSyn can induce a robust lesion of the nigrostriatal system leading to behavioral phenotypes in rodents and non-human primates using a system that allows spatiotemporal control and the ability to design studies with an internal control [23][23]. In addition, the level of protein overexpression can easily be altered to reduce the level of overexpression to sub-toxic levels or prolong the time before degeneration if desired [14,24–25]. The main drawback of this model, however, is the supra-physiological level of overexpression required for pathology, leading to the question of generalizability between this model and the human condition.…”

Section: Common Methods For Modeling Parkinson’s Disease In Rodentsmentioning

confidence: 99%

Best Practices for Generating and Using Alpha-Synuclein Pre-Formed Fibrils to Model Parkinson’s Disease in Rodents

Polinski

Volpicelli‐Daley

Sortwell

et al. 2018

JPD

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185

197

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Parkinson’s disease (PD) is the second most common neurodegenerative disease, affecting approximately one-percent of the population over the age of sixty. Although many animal models have been developed to study this disease, each model presents its own advantages and caveats. A unique new model has arisen to study the role of alpha-synuclein (aSyn) in the pathogenesis of PD. This model involves the conversion of recombinant monomeric aSyn protein to a fibrillar form—the aSyn pre-formed fibril (aSyn PFF)—which is then injected into the brain or introduced to the media in culture. Although many groups have successfully adopted and replicated the aSyn PFF model, issues with generating consistent pathology have been reported by investigators. To improve the replicability of this model and diminish these issues, The Michael J. Fox Foundation for Parkinson’s Research (MJFF) has enlisted the help of field leaders who performed key experiments to establish the aSyn PFF model to provide the research community with guidelines and practical tips for improving the robustness and success of this model. Specifically, we identify key pitfalls and suggestions for avoiding these mistakes as they relate to generating the aSyn PFFs from monomeric protein, validating the formation of pathogenic aSyn PFFs, and using the aSyn PFFs in vivo or in vitro to model PD. With this additional information, adoption and use of the aSyn PFF model should present fewer challenges, resulting in a robust and widely available model of PD.

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Back and to the Future: From Neurotoxin‐Induced to Human Parkinson's Disease Models

et al. 2020

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Parkinson's disease (PD) is an age‐related neurodegenerative disorder characterized by motor symptoms such as tremor, slowness of movement, rigidity, and postural instability, as well as non‐motor features like sleep disturbances, loss of ability to smell, depression, constipation, and pain. Motor symptoms are caused by depletion of dopamine in the striatum due to the progressive loss of dopamine neurons in the substantia nigra pars compacta. Approximately 10% of PD cases are familial arising from genetic mutations in α‐synuclein, LRRK2, DJ‐1, PINK1, parkin, and several other proteins. The majority of PD cases are, however, idiopathic, i.e., having no clear etiology. PD is characterized by progressive accumulation of insoluble inclusions, known as Lewy bodies, mostly composed of α‐synuclein and membrane components. The cause of PD is currently attributed to cellular proteostasis deregulation and mitochondrial dysfunction, which are likely interdependent. In addition, neuroinflammation is present in brains of PD patients, but whether it is the cause or consequence of neurodegeneration remains to be studied. Rodents do not develop PD or PD‐like motor symptoms spontaneously; however, neurotoxins, genetic mutations, viral vector‐mediated transgene expression and, recently, injections of misfolded α‐synuclein have been successfully utilized to model certain aspects of the disease. Here, we critically review the advantages and drawbacks of rodent PD models and discuss approaches to advance pre‐clinical PD research towards successful disease‐modifying therapy. © 2020 The Authors.

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Morphological and Behavioral Impact of AAV2/5-Mediated Overexpression of Human Wildtype Alpha-Synuclein in the Rat Nigrostriatal System

Cited by 75 publications

References 57 publications

Recombinant adenoassociated virus 2/5-mediated gene transfer is reduced in the aged rat midbrain

Recombinant adenoassociated virus 2/5-mediated gene transfer is reduced in the aged rat midbrain

Best Practices for Generating and Using Alpha-Synuclein Pre-Formed Fibrils to Model Parkinson’s Disease in Rodents

Back and to the Future: From Neurotoxin‐Induced to Human Parkinson's Disease Models

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