| Literature DB >> 32994544 |
Sara Dominguez1, Eugene Varfolomeev2, Robert Brendza1, Kim Stark1, Joy Tea1, Jose Imperio1, Hai Ngu3, Timothy Earr1, Oded Foreman3, Joshua D Webster3, Amy Easton1, Domagoj Vucic2, Baris Bingol4.
Abstract
RIP1 kinase is proposed to play a critical role in driving necroptosis and inflammation in neurodegenerative disorders, including Amyotrophic Lateral Sclerosis (ALS). Preclinical studies indicated that while pharmacological inhibition of RIP1 kinase can ameliorate axonal pathology and delay disease onset in the mutant SOD1 transgenic (SOD1-Tg) mice, genetic blockade of necroptosis does not provide benefit in this mouse model. To clarify the role of RIP1 kinase activity in driving pathology in SOD1-Tg mice, we crossed SOD1-Tgs to RIP1 kinase-dead knock-in mice, and measured disease progression using functional and histopathological endpoints. Genetic inactivation of the RIP1 kinase activity in the SOD1-Tgs did not benefit the declining muscle strength or nerve function, motor neuron degeneration or neuroinflammation. In addition, we did not find evidence of phosphorylated RIP1 accumulation in the spinal cords of ALS patients. On the other hand, genetic inactivation of RIP1 kinase activity ameliorated the depletion of the neurotransmitter dopamine in a toxin model of dopaminergic neurodegeneration. These findings indicate that RIP1 kinase activity is dispensable for disease pathogenesis in the SOD1-Tg mice while inhibition of kinase activity may provide benefit in acute injury models.Entities:
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Year: 2020 PMID: 32994544 PMCID: PMC7937687 DOI: 10.1038/s41418-020-00625-7
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 15.828