In the mdx mouse model of Duchenne muscular dystrophy, in vivo reduction of microtubule detyrosination with LC-1 protected against workload-induced arrhythmias and contraction-induced skeletal muscle injury.
Does pharmacological reduction of detyrosination prevent aberrant X-ROS signalling and workload-induced arrhythmias in the mdx mouse model of DMD?
Targeting detyrosination of microtubules reduces aberrant mechanotransduction and protects against arrhythmias and muscle injury in a mouse model of Duchenne muscular dystrophy.
Tasa de eventos absoluta: 100% vs 7.6%
valor p: p=<0.05
In striated muscle, X-ROS is the mechanotransduction pathway by which mechanical stress transduced by the microtubule network elicits reactive oxygen species. X-ROS tunes Ca(2+) signalling in healthy muscle, but in diseases such as Duchenne muscular dystrophy (DMD), microtubule alterations drive elevated X-ROS, disrupting Ca(2+) homeostasis and impairing function. Here we show that detyrosination, a post-translational modification of α-tubulin, influences X-ROS signalling, contraction speed and cytoskeletal mechanics. In the mdx mouse model of DMD, the pharmacological reduction of detyrosination in vitro ablates aberrant X-ROS and Ca(2+) signalling, and in vivo it protects against hallmarks of DMD, including workload-induced arrhythmias and contraction-induced injury in skeletal muscle. We conclude that detyrosinated microtubules increase cytoskeletal stiffness and mechanotransduction in striated muscle and that targeting this post-translational modification may have broad therapeutic potential in muscular dystrophies.
Kerr et al. (Thu,) conducted a other in Duchenne muscular dystrophy. Parthenolide (PTL) / LC-1 vs. Vehicle / DMSO was evaluated on Survival following isoproterenol challenge in mdx mice (p=<0.05). In the mdx mouse model of Duchenne muscular dystrophy, in vivo reduction of microtubule detyrosination with LC-1 protected against workload-induced arrhythmias and contraction-induced skeletal muscle injury.
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