MicroRNA may serve as therapeutic targets for traumatic brain injury

(Walter Reed Army Institute of Research) WRAIR scientists have shown that traumatic brain injury causes coordinated microRNA dysregulation followed by increased amounts of the beta-site amyloid cleaving enzyme, or BACE1, and loss of amyloid precursor protein. BACE-1 cleaves APP to generate amyloid beta peptides, a hallmark of neurodegenerative disease pathology and brain cells loss, which are the focus of several clinical trials for Alzheimer's disease. Future research will characterize the direct role of miRNAs and their relationship to BACE1 within TBI.
Source: EurekAlert! - Medicine and Health - Category: International Medicine & Public Health Source Type: news