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Primary progressive aphasia and motor neuron disease: A review

Authors :
Aiello, E
Feroldi, S
De Luca, G
Guidotti, L
Arrigoni, E
Appollonio, I
Solca, F
Carelli, L
Poletti, B
Verde, F
Silani, V
Ticozzi, N
Aiello E. N.
Feroldi S.
De Luca G.
Guidotti L.
Arrigoni E.
Appollonio I.
Solca F.
Carelli L.
Poletti B.
Verde F.
Silani V.
Ticozzi N.
Aiello, E
Feroldi, S
De Luca, G
Guidotti, L
Arrigoni, E
Appollonio, I
Solca, F
Carelli, L
Poletti, B
Verde, F
Silani, V
Ticozzi, N
Aiello E. N.
Feroldi S.
De Luca G.
Guidotti L.
Arrigoni E.
Appollonio I.
Solca F.
Carelli L.
Poletti B.
Verde F.
Silani V.
Ticozzi N.
Publication Year :
2022

Abstract

Background: This study aims at reviewing, within the framework of motor neuron disease-frontotemporal degeneration (MND-FTD)-spectrum disorders, evidence on the co-occurrence between primary progressive aphasia (PPA) and MND in order to profile such a complex at pathological, genetic and clinical levels. Methods: This review was pre-registered (osf.io/ds8m4) and performed in accordance with the 2020 PRISMA guidelines. Case reports/series and group studies were included if addressing (1) progressive non-fluent aphasia (PNFA) or semantic dementia (SD) with MND or (2) MND patients with co-morbid PNFA/SD. Results: Out of 546 initial records, 56 studies were included. As to case reports/series (N = 35), which included 61 PPA-MND patients, the following findings yielded: (1) PNFA is more frequent than SD in PPA-MND; (2) in PPA-MND, the most prevalent motor phenotypes are amyotrophic lateral sclerosis and predominant-upper MND, with bulbar involvement being ubiquitous; (3) extrapyramidal features are moderately frequent in PPA-MND; (4) PPA-MND patients usually display frontotemporal, left-greater-than-right involvement; (5) TDP-43-B is the typical pathological substrate of PPA-MND; (6) TBK1 mutations represent the most frequent genetic risk factors for PPA-MND. As to group studies, including 121 patients, proportional meta-analytic procedures revealed that: (1) the lifetime prevalence of MND in PPA is 6%; (2) PPA occurs in 19% of patients with co-morbid MND and FTD; (3) MND is more frequent in PNFA (10%) than in SD patients (3%). Discussion: Insights herewith delivered into the clinical, neuropathological and genetic features of PPA-MND patients prompt further investigations aimed at improving clinical practice within the MND-FTD spectrum.

Details

Database :
OAIster
Notes :
ELETTRONICO, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1350082315
Document Type :
Electronic Resource