Modulating rapamycin target protein promotes autophagy, lowering toxic Huntingtin protein

(Buck Institute for Research on Aging) Recent failed clinical trials of a drug designed to clear the mutant Huntingtin protein that causes Huntington's disease (HD) heightens the need for new approaches for the devastating, incurable, progressive neurodegenerative genetic disorder. Scientists at the Buck Institute have found that the targeting the protein called FK506-binding protein 51 or FKBP51 promotes the clearing of those toxic proteins via autophagy, a natural process whereby cells recycle damaged proteins and mitochondria and use them for nutrition.
Source: EurekAlert! - Medicine and Health - Category: International Medicine & Public Health Source Type: news