| Literature DB >> 29525180 |
Anna Bartoletti-Stella1, Simone Baiardi2, Michelangelo Stanzani-Maserati3, Silvia Piras3, Paolo Caffarra4, Alberto Raggi5, Roberta Pantieri3, Sara Baldassari3, Leonardo Caporali3, Samir Abu-Rumeileh2, Simona Linarello6, Rocco Liguori7, Piero Parchi8, Sabina Capellari9.
Abstract
Genetics is intricately involved in the etiology of neurodegenerative dementias. The incidence of monogenic dementia among all neurodegenerative forms is unknown due to the lack of systematic studies and of patient/clinician access to extensive diagnostic procedures. In this study, we conducted targeted sequencing in 246 clinically heterogeneous patients, mainly with early-onset and/or familial neurodegenerative dementia, using a custom-designed next-generation sequencing panel covering 27 genes known to harbor mutations that can cause different types of dementia, in addition to the detection of C9orf72 repeat expansions. Forty-nine patients (19.9%) carried known pathogenic or novel, likely pathogenic, variants, involving both common (presenilin 1, presenilin 2, C9orf72, and granulin) and rare (optineurin, serpin family I member 1 and protein kinase cyclic adenosine monophosphate (cAMP)-dependent type I regulatory subunit beta) dementia-associated genes. Our results support the use of an extended next-generation sequencing panels as a quick, accurate, and cost-effective method for diagnosis in clinical practice. This approach could have a significant impact on the proportion of tested patients, especially among those with an early disease onset.Entities:
Keywords: C9orf72 RE; Double mutations; Familial dementia; Neurodegenerative dementia; Next-generation sequencing; Targeted gene sequencing
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Year: 2018 PMID: 29525180 DOI: 10.1016/j.neurobiolaging.2018.02.006
Source DB: PubMed Journal: Neurobiol Aging ISSN: 0197-4580 Impact factor: 4.673