Screen for MURF-1 inhibitors to treat myopathy
Mattern, Michael R.   
Progenra, Inc., Malvern, PA, United States

Myopathy (muscle atrophy, or muscle wasting) is a serious clinical complication of cancer, HIV/AIDS, diabetes, and other chronic diseases, leading to increased morbidity and reduced life expectancy. While symptoms have been addressed by a number of interventions, no successful therapy has been developed. Recently, various proteins whose expression is enhanced under conditions of atrophy-inducing starvation have been identified in rats. In particular, the expression of a set of novel genes called atrogins (atrophyspecific genes) increases significantly in skeletal muscles of fasting organisms and decreases rapidly when feeding is resumed. The product of one of these genes - MURF-1 - is RING-finger domain ubiquitin E3 ligase, a critical enzyme of the ubiquitin-proteasomal degradation pathway. Genetic knockout and pharmacological studies have implicated this pathway in muscle atrophy. Thus, attenuation of proteasomal activity associated with muscle wasting may be achievable using inhibitors of MURF-1. In Phase I, E3 ubiquitination activity of MURF-1 will be demonstrated against an appropriate substrate. Then, a yeastbased assay for inhibitors of MURF-1 will be developed and validated, and a collection of natural products extracts will be screened. For the assay, the following will be cloned and expressed in yeast S. cerevisiae: the substrate of MURF-1, fused to p53 linked to a (3-galactosidase reporter; free MURF-1 (E3 ligase); an E3 ligase suitable as a selectivity control. After the assay is adapted to multiwell plates and to parameters acceptable for high throughput screening, a collection of natural product extracts and a set of screening compounds from the NCI will be screened for inhibitors of MURF-1. Successful completion of Phase I should result in at least one extract lead with reasonable potency (IC50 1-5 ug/ml). In Phase II, active principles will be isolated from the best extract leads and best hits from the small molecule screen will be selected for lead optimization, with the goal of identifying novel, potent, and selective inhibitors of MURF-1 for development as therapies for muscle wasting associated with various pathological states.