The rho kinase inhibitor Y-27632 improves motor performance in male SOD1(G93A) mice

2014 | journal article; research paper. A publication with affiliation to the University of Göttingen.

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​The rho kinase inhibitor Y-27632 improves motor performance in male SOD1(G93A) mice​
Günther, R. ; Saal, K.-A. ; Suhr, M. ; Scheer, D.; Koch, J. C. ; Bähr, M.   & Lingor, P.  et al.​ (2014) 
Frontiers in Neuroscience8 art. 304​.​ DOI: https://doi.org/10.3389/fnins.2014.00304 

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Authors
Günther, R. ; Saal, K.-A. ; Suhr, M. ; Scheer, D.; Koch, J. C. ; Bähr, M. ; Lingor, P. ; Tönges, L. 
Abstract
Disease progression in amyotrophic lateral sclerosis (ALS) is characterized by degeneration of motoneurons and their axons which results in a progressive muscle weakness and ultimately death from respiratory failure. The only approved drug, riluzole, lacks clinical efficacy so that more potent treatment options are needed. We have identified rho kinase (ROCK) as a target, which can be manipulated to beneficially influence disease progression in models of ALS. Here, we examined the therapeutic potential of the ROCK inhibitor Y-27632 in both an in vitro and in an in vivo paradigm of motoneuron disease. Application of Y-27632 to primary motoneurons in vitro increased survival and promoted neunte outgrowth. In vivo, SOD1G93A mice were orally treated with 2 or 30 mg/kg body weight of Y-27632. The 2 mg/kg group did not benefit from Y-27632 treatment, whereas treatment with 30 mg/kg resulted in improved motor function in male mice. Female mice showed only limited improvement and overall survival was not modified in both 2 and 30 mg/kg Y-27632 groups. In conclusion, we provide evidence that inhibition of ROCK by Y-27632 is neuroprotective in vitro but has limited beneficial effects in vivo being restricted to male mice. Therefore, the evaluation of ROCK inhibitors in preclinical models of ALS should always take gender differences into account.
Issue Date
2014
Journal
Frontiers in Neuroscience 
ISSN
1662-453X
Extent
9
Language
English

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