Preclinical Amyotrophic Lateral Sclerosis (ALS) Studies to Advance Your Research

PsychoGenics leverages transgenic models to advance preclinical studies of amyotrophic lateral sclerosis (ALS), a progressive paralytic disorder characterized by motor neuron degeneration in the brain and spinal cord. Our expertise extends to both sporadic (SALS) and familial (FALS) forms of ALS, with a particular focus on mutations in the superoxide dismutase 1 (SOD1) and TDP-43.

Progressive weight loss in the ∆rNLS8 mice once Dox is removed.

Survival is decreased in the ∆rNLS8 mice after DOX removal.

Tremor and Hindlimb Clasping

rNLS8 mice show tremors following DOX removal. These tremors are absent when mice are kept on DOX chow.

rNLS8 mice exhibit hindlimb clasping after DOX removal. This behavior is not observed in the presence of DOX.

rNLS8 mice show progressive weakness in the wire hang test and fall quicker compared to the tTA mice. Deficits are seen within 2 weeks after DOX removal.

NLS8 mice fall quicker from a rotating rod compared to tTA mice. The deficits in rotarod performance is seen as early as 1 week post DOX removal.

rNLS mice show an increase in the onset latency of muscle activation in response to motor nerve stimulation4 weeks post DOX removal.

rNLS mice show a decrease in response amplitude 4 weeks post DOX removal.

rNLS mice show a decrease in muscle nerve conduction 4 weeks post DOX removal.

rNLS8 mice show age-dependent elevation of plasma NF-L levels following cessation of DOX treatment.

rNLS8 mice show age-dependent elevated CSF NF-L levels following cessation of DOX treatment.