Minimum Effective Dose of Clemastine in a Mouse Model of Preterm White Matter Injury.

Elizabeth OdellNora JabassiniBjörn SchniedewindSarah E Pease-RaissiAdam FrymoyerUwe ChristiansAri J GreenJonah R Chan Bridget Elaine LaMonica Ostrem

Published in: bioRxiv : the preprint server for biology (2024)

Preterm white matter injury (PWMI) is the most common cause of brain injury and cerebral palsy in premature neonates.Clemastine, an FDA-approved antihistamine, was recently identified to strongly promote myelination in a mouse model of PWMI and is a possible treatment.The minimum effective dose in neonatal rodents is unknown and is critical for guiding dose selection and balancing efficacy with toxicity in future clinical trials.We identified the minimum effective dose of clemastine and the associated pharmacokinetics in a murine chronic hypoxia model of PWMI, paving the way for a future clinical trial in human neonates.

Keyphrases

clinical trial
brain injury
white matter
mouse model
low birth weight
cerebral palsy
endothelial cells
subarachnoid hemorrhage
multiple sclerosis
preterm birth
current status
preterm infants
phase ii
open label
study protocol
randomized controlled trial