Novel chronic mouse model of cerebral cavernous malformations
C Cardoso, M Arnould, C De Luca, C Otten… - Stroke, 2020 - Am Heart Assoc
C Cardoso, M Arnould, C De Luca, C Otten, S Abdelilah-Seyfried, A Heredia…
Stroke, 2020•Am Heart AssocBackground and Purpose—Cerebral cavernous malformations (CCMs) are vascular
malformations of the brain that lead to cerebral hemorrhages. A pharmacological treatment
is needed especially for patients with nonoperable deep-seated lesions. We and others
obtained CCM mouse models that were useful for mechanistic studies and rapid trials
testing the preventive effects of candidate drugs. The shortened lifespan of acute mouse
models hampered evaluation of compounds that would not only prevent lesion appearance …
malformations of the brain that lead to cerebral hemorrhages. A pharmacological treatment
is needed especially for patients with nonoperable deep-seated lesions. We and others
obtained CCM mouse models that were useful for mechanistic studies and rapid trials
testing the preventive effects of candidate drugs. The shortened lifespan of acute mouse
models hampered evaluation of compounds that would not only prevent lesion appearance …
Background and Purpose
Cerebral cavernous malformations (CCMs) are vascular malformations of the brain that lead to cerebral hemorrhages. A pharmacological treatment is needed especially for patients with nonoperable deep-seated lesions. We and others obtained CCM mouse models that were useful for mechanistic studies and rapid trials testing the preventive effects of candidate drugs. The shortened lifespan of acute mouse models hampered evaluation of compounds that would not only prevent lesion appearance but also cure preexisting lesions. Indirubin-3′-monoxime previously demonstrated its efficacy to reverse the cardiac phenotype of ccm2m201 zebrafish mutants and to prevent lesion development in an acute CCM2 mouse model. In the present article, we developed and characterized a novel chronic CCM2 mouse model and evaluated the curative therapeutic effect of indirubin-3′-monoxime after CCM lesion development.
Methods
The chronic mouse model was obtained by a postnatal induction of brain-endothelial-cell-specific ablation of the Ccm2 gene using the inducible Slco1c1-CreERT2 mouse line.
Results
We obtained a fully penetrant novel CCM chronic mouse model without any obvious off-target phenotypes and compatible with long-term survival. By 3 months of age, CCM lesions ranging in size from small isolated lesions to multiple caverns developed throughout the brain. Lesion burden was quantified in animals from 1 week to 5 months of age. Clear signs of intracerebral hemorrhages were noticed in brain-endothelial-cell-specific ablation of the Ccm2 gene. In contrast with its preventive effect in the acute CCM2 mouse model, a 20 mg/kg indirubin-3′-monoxime treatment for 3 weeks in 3-month old animals neither had any beneficial effect on the lesion burden nor alleviated cerebral hemorrhages.
Conclusions
The brain-endothelial-cell-specific ablation of the Ccm2 gene chronic model is a strongly improved disease model for the CCM community whose challenge today is to decipher which candidate drugs might have a curative effect on patients’ preexisting lesions.
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