Longitudinal clinical, neuropsychological, and neuroimaging characterization of a kindred with a 12-octapeptide repeat insertion in

IMPORTANCE: Highly penetrant inherited mutations in the prion protein gene (PRNP) offer a window to study the pathobiology of prion disorders. OBJECTIVE: To characterize the longitudinal clinical features, neuropsychological findings, MRI findings, and FGD-PET scan imaging findings in a subsequent generation of a family with a large 12-octapeptide repeat insertion in the PRNP gene. DESIGN: Clinical, neuropsychological, and neuroimaging characterization of a kindred. SETTING: Mayo Clinic Alzheimer Disease Research Center (Rochester, Minnesota). PARTICIPANTS: Four mutation carriers and two non-carriers in the third generation of a kindred with a large octapeptide repeat insertion in the PRNP gene. RESULTS: Three of the four mutation carriers have progressed to a frontotemporal dementia phenotype. Declines in neuropsychological function coincided with changes in FDG-PET at the identified onset of cognitive impairment. Processing speed and executive function were abnormal before the identified onset. CONCLUSIONS AND RELEVANCE: Gene silencing treatments are on the horizon and when they become available, early detection will be crucial. Longitudinal studies involving familial mutation kindreds can offer important insights into the initial neuropsychological and neuroimaging changes necessary for early detection.