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Identification of novel and disease-related VCP/p97 binding partners and effects of disease-causing VCP/p97 mutations on protein interactions and protein quality control systems in Dictyostelium and mouse

Subject Area Molecular and Cellular Neurology and Neuropathology
Term from 2009 to 2018
Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 101925924
 
Mutations of the human VCP/p97 gene cause autosomal dominant "Inclusion Body Myopathy with early-onset Paget disease of bone and Frontotemporal Dementia" (IBMPFD) and an "amyotrophic lateral sclerosis" (ALS) variant. In the first funding period, we generated and characterized a series of VCP/p97 mutant Dictyostelium strains, characterized a VCP/p97 haploinsufficient mouse model and identified and characterized novel and disease-relevant VCP/p97 binding partners. In the proposed work program for the second funding period, we will extend our studies on VCP/p97 with particular emphasis on the molecular basis of IBMPFD, employing a broad spectrum of experimental procedures ranging from biochemical and molecular biology experiments, cell biological assays using mammalian and Dictyostelium cells to mouse models. We will identify further novel VCP/p97 binding partners, explore the molecular interactions within VCP/p97 protein complexes and analyze expression changes in autophagy components. We will elucidate functional consequences of R155C mutant VCP/p97 in Dictyostelium strains with respect to proteasomal activity, autophagy flux, and the composition of protein aggregates. Corresponding experiments as well as a detailed characterization of the skeletal muscle pathology will be carried out in our newly generated R155C VCP/p97 knock-in mouse model.
DFG Programme Research Units
 
 

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