New immunotherapeutic agent for the treatment of Alzheimer's disease.

The toxic amyloid-beta (Abeta) peptides involved in Alzheimer’s disease (AD) are produced after processing of the amyloid precursor protein-C-terminal fragment APP-C99 by gamma-secretase. Thus, major therapeutic efforts have been focused on inhibiting the activity of this enzyme. However, recent human phase 3 clinical trials testing gamma-secretase inhibitors revealed adverse side effects attributed to impaired processing of the Notch-1 receptor, a gamma-secretase substrate critically involved in cell fate decisions. Here, the group of Prof. Patrick Fraering (CMSN – Molecular and Cellular Biology of Alzheimer's Disease) report an innovative approach to selectively target the gamma-secretase-mediated processing of APP-C99 with monoclonal antibodies neutralizing this substrate. Generated by immunizing mice with natively folded APP-C99, these antibodies bind native epitopes of this substrate, and by steric hindrance significantly reduce Abeta production in cells as well as in a mouse model of AD. Together, these findings support APP-C99 substrate-targeting antibodies as new immunotherapeutic and Notch-sparing agents to lower the levels of Abeta peptides implicated in AD.

Jemila Houacine et al., Neurobiology of Aging, http://dx.doi.org/10.1016/j.neurobiolaging.2011.12.033 (2012)