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α-Synuclein–induced Kv4 channelopathy in mouse vagal motoneurons drives nonmotor parkinsonian symptoms

Wei‐Hua Chiu, Lora Kovacheva, Ruth E. Musgrove, Hadar Arien‐Zakay, James B. Koprich, Jonathan M. Brotchie, Rami Yaka, Danny Ben‐Zvi, Menachem Hanani, Jochen Roeper, Joshua A. Goldberg

2021Science Advances20 citationsDOIOpen Access PDF

Abstract

No disease-modifying therapy is currently available for Parkinson's disease (PD), the second most common neurodegenerative disease. The long nonmotor prodromal phase of PD is a window of opportunity for early detection and intervention. However, we lack the pathophysiological understanding to develop selective biomarkers and interventions. By using a mutant α-synuclein selective-overexpression mouse model of prodromal PD, we identified a cell-autonomous selective Kv4 channelopathy in dorsal motor nucleus of the vagus (DMV) neurons. This functional remodeling of intact DMV neurons leads to impaired pacemaker function in vitro and in vivo, which, in turn, reduces gastrointestinal motility, a common early symptom of prodromal PD. We identify a chain of events from α-synuclein via a biophysical dysfunction of a specific neuronal population to a clinically relevant prodromal symptom. These findings will facilitate the rational design of clinical biomarkers to identify people at risk for developing PD.

Topics & Concepts

ChannelopathyNeuroscienceBiologyMedicineParkinson's Disease Mechanisms and TreatmentsBotulinum Toxin and Related Neurological DisordersNeurological disorders and treatments
α-Synuclein–induced Kv4 channelopathy in mouse vagal motoneurons drives nonmotor parkinsonian symptoms | Litcius