Mutations in the PRKN gene encoding the protein parkin cause autosomal recessive juvenile parkinsonism (ARJP). Harnessing this mutation to create an early-onset Parkinson's disease mouse model would provide a unique opportunity to clarify the mechanisms involved in the neurodegenerative process and lay the groundwork for the development of neuroprotective strategies. To this end, we created a knock-in mouse carrying the homozygous PrknR275W mutation, which is the missense mutation with the highest allelic frequency in PRKN patients. We evaluated the anatomical and functional integrity of the nigrostriatal dopamine (DA) pathway, as well as motor behaviour in PrknR275W mice of both sexes.We report here that PrknR275W mice show early DA neuron dysfunction, age-dependent loss of DA neurons in the substantia nigra, decreased DA content and stimulus-evoked DA release in the striatum, and progressive motor impairment. Together, these data show that the PrknR275W mouse recapitulates key features of ARJP. Thus, these studies fill a critical need in the field by introducing a promising new Parkinson's disease model in which to study causative mechanisms of the disease and test therapeutic strategies.Mutations in the PRKN gene are the most common cause of autosomal recessive juvenile parkinsonism (ARJP). Regoni et al. create a new mouse model of ARJP that recapitulates key features of the human disease, providing a means of studying casual mechanisms and testing therapeutic strategies.
Dopamine neuron dysfunction and loss in the PrknR275W mouse model of juvenile parkinsonism / Regoni, Maria; Zanetti, Letizia; Sevegnani, Martina; Domenicale, Chiara; Magnabosco, Stefano; Patel, Jyoti C; Fernandes, Megan K; Feeley, Ryan M; Monzani, Elena; Mini, Cecilia; Comai, Stefano; Cherchi, Laura; De Gregorio, Danilo; Soliman, Isabella; Ruto, Fabio; Croci, Laura; Consalez, Giacomo; Rodighiero, Simona; Ciammola, Andrea; Valtorta, Flavia; Morari, Michele; Piccoli, Giovanni; Rice, Margaret E; Sassone, Jenny. - In: BRAIN. - ISSN 0006-8950. - (2024). [10.1093/brain/awae276]
Dopamine neuron dysfunction and loss in the PrknR275W mouse model of juvenile parkinsonism
Regoni, Maria;Zanetti, Letizia;Comai, Stefano;De Gregorio, Danilo;Ruto, Fabio;Consalez, Giacomo;Valtorta, Flavia;Piccoli, Giovanni;Sassone, Jenny
2024-01-01
Abstract
Mutations in the PRKN gene encoding the protein parkin cause autosomal recessive juvenile parkinsonism (ARJP). Harnessing this mutation to create an early-onset Parkinson's disease mouse model would provide a unique opportunity to clarify the mechanisms involved in the neurodegenerative process and lay the groundwork for the development of neuroprotective strategies. To this end, we created a knock-in mouse carrying the homozygous PrknR275W mutation, which is the missense mutation with the highest allelic frequency in PRKN patients. We evaluated the anatomical and functional integrity of the nigrostriatal dopamine (DA) pathway, as well as motor behaviour in PrknR275W mice of both sexes.We report here that PrknR275W mice show early DA neuron dysfunction, age-dependent loss of DA neurons in the substantia nigra, decreased DA content and stimulus-evoked DA release in the striatum, and progressive motor impairment. Together, these data show that the PrknR275W mouse recapitulates key features of ARJP. Thus, these studies fill a critical need in the field by introducing a promising new Parkinson's disease model in which to study causative mechanisms of the disease and test therapeutic strategies.Mutations in the PRKN gene are the most common cause of autosomal recessive juvenile parkinsonism (ARJP). Regoni et al. create a new mouse model of ARJP that recapitulates key features of the human disease, providing a means of studying casual mechanisms and testing therapeutic strategies.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
