Longitudinal MRI and 1H-MRS study of SCA7 mouse forebrain reveals progressive multiregional atrophy and early brain metabolite changes indicating early neuronal and glial dysfunction

Pérot, Jean-Baptiste; Niewiadomska-Cimicka, Anna; Brouillet, Emmanuel; Trottier, Yvon; Flament, Julien

doi:10.1371/journal.pone.0296790

Cited by 2 publications

(1 citation statement)

References 38 publications

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“…Although the cerebellum is a major target for therapeutic development in ataxias, other brain structures are often affected and must also be considered. Recent magnetic resonance imaging of SCA7 mice revealed progressive atrophy of several forebrain regions, including the striatum and hippocampus [42]. We found that systemic injection of AAV PHP.eB efficiently transduced the striatum and hippocampus and led to a reduction of mATXN7 level (by 56% and 39%, respectively) by shA4 treatment.…”

Section: Efficacy and Limitation Of Aav Phpeb Serotype For Preclinica...mentioning

confidence: 71%

AAV-Mediated CAG-Targeting Selectively Reduces Polyglutamine-Expanded Protein and Attenuates Disease Phenotypes in a Spinocerebellar Ataxia Mouse Model

Niewiadomska-Cimicka,

Fievet,

Surdyka

et al. 2024

IJMS

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Polyglutamine (polyQ)-encoding CAG repeat expansions represent a common disease-causing mutation responsible for several dominant spinocerebellar ataxias (SCAs). PolyQ-expanded SCA proteins are toxic for cerebellar neurons, with Purkinje cells (PCs) being the most vulnerable. RNA interference (RNAi) reagents targeting transcripts with expanded CAG reduce the level of various mutant SCA proteins in an allele-selective manner in vitro and represent promising universal tools for treating multiple CAG/polyQ SCAs. However, it remains unclear whether the therapeutic targeting of CAG expansion can be achieved in vivo and if it can ameliorate cerebellar functions. Here, using a mouse model of SCA7 expressing a mutant Atxn7 allele with 140 CAGs, we examined the efficacy of short hairpin RNAs (shRNAs) targeting CAG repeats expressed from PHP.eB adeno-associated virus vectors (AAVs), which were introduced into the brain via intravascular injection. We demonstrated that shRNAs carrying various mismatches with the CAG target sequence reduced the level of polyQ-expanded ATXN7 in the cerebellum, albeit with varying degrees of allele selectivity and safety profile. An shRNA named A4 potently reduced the level of polyQ-expanded ATXN7, with no effect on normal ATXN7 levels and no adverse side effects. Furthermore, A4 shRNA treatment improved a range of motor and behavioral parameters 23 weeks after AAV injection and attenuated the disease burden of PCs by preventing the downregulation of several PC-type-specific genes. Our results show the feasibility of the selective targeting of CAG expansion in the cerebellum using a blood–brain barrier-permeable vector to attenuate the disease phenotype in an SCA mouse model. Our study represents a significant advancement in developing CAG-targeting strategies as a potential therapy for SCA7 and possibly other CAG/polyQ SCAs.

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Section: Efficacy and Limitation Of Aav Phpeb Serotype For Preclinica...mentioning

confidence: 71%

AAV-Mediated CAG-Targeting Selectively Reduces Polyglutamine-Expanded Protein and Attenuates Disease Phenotypes in a Spinocerebellar Ataxia Mouse Model

Niewiadomska-Cimicka,

Fievet,

Surdyka

et al. 2024

IJMS

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NMR in living systems

Prior

2024

Nuclear Magnetic Resonance

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This chapter reviews studies published during the period of May 2023 to April 2024 that have applied magnetic resonance spectroscopy to investigate processes occurring in living systems. In Section 1, new hardware, acquisition methods and analytical processes that are applicable to in vivo investigations are presented. Studies in pre-clinical models and the clinical environment are surveyed in Sections 2 and 3, respectively. The review in both these two sections is subdivided into physiological categories, with each of these sub-divided according to the category of disease or the type of metabolic investigation.

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Longitudinal MRI and 1H-MRS study of SCA7 mouse forebrain reveals progressive multiregional atrophy and early brain metabolite changes indicating early neuronal and glial dysfunction

Cited by 2 publications

References 38 publications

AAV-Mediated CAG-Targeting Selectively Reduces Polyglutamine-Expanded Protein and Attenuates Disease Phenotypes in a Spinocerebellar Ataxia Mouse Model

AAV-Mediated CAG-Targeting Selectively Reduces Polyglutamine-Expanded Protein and Attenuates Disease Phenotypes in a Spinocerebellar Ataxia Mouse Model

NMR in living systems

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