Can MRI Visual Assessment Differentiate the Variants of Primary-Progressive Aphasia?

S A Sajjadi; N Sheikh-Bahaei; J Cross; J H Gillard; D Scoffings; P J Nestor

doi:10.3174/ajnr.A5126

Can MRI Visual Assessment Differentiate the Variants of Primary-Progressive Aphasia?

AJNR Am J Neuroradiol. 2017 May;38(5):954-960. doi: 10.3174/ajnr.A5126. Epub 2017 Mar 24.

Authors

S A Sajjadi¹, N Sheikh-Bahaei^{2

3}, J Cross³, J H Gillard^{2

3}, D Scoffings³, P J Nestor⁴

Affiliations

¹ From the Department of Neurology (S.A.S.), University of California, Irvine, Irvine, California ssajjadi@uci.edu.
² Department of Radiology (N.S.-B., J.H.G.), University of Cambridge, Cambridge, UK.
³ Department of Radiology (N.S.-.B., J.C., J.H.G., D.S.), Cambridge University Hospitals, Cambridge, UK.
⁴ German Center for Neurodegenerative Diseases (P.J.N.), Magdeburg, Germany.

Abstract

Background and purpose: Primary-progressive aphasia is a clinically and pathologically heterogeneous condition. Nonfluent, semantic, and logopenic are the currently recognized clinical variants. The recommendations for the classification of primary-progressive aphasia have advocated variant-specific patterns of atrophy. The aims of the present study were to evaluate the sensitivity and specificity of the proposed imaging criteria and to assess the intra- and interrater reporting agreements.

Materials and methods: The cohort comprised 51 patients with a root diagnosis of primary-progressive aphasia, 25 patients with typical Alzheimer disease, and 26 matched control participants. Group-level analysis (voxel-based morphometry) confirmed the proposed atrophy patterns for the 3 syndromes. The individual T1-weighted anatomic images were reported by 3 senior neuroradiologists.

Results: We observed a dichotomized pattern of high sensitivity (92%) and specificity (93%) for the proposed atrophy pattern of semantic-variant primary-progressive aphasia and low sensitivity (21% for nonfluent-variant primary-progressive aphasia and 43% for logopenic-variant primary-progressive aphasia) but high specificity (91% for nonfluent-variant primary-progressive aphasia and 95% for logopenic-variant primary-progressive aphasia) in other primary-progressive aphasia variants and Alzheimer disease (sensitivity 43%, specificity 92%). MR imaging was least sensitive for the diagnosis of nonfluent-variant primary-progressive aphasia. Intrarater agreement analysis showed mean κ values above the widely accepted threshold of 0.6 (mean, 0.63 ± 0.16). Pair-wise interobserver agreement outcomes, however, were well below this threshold in 5 of the 6 possible interrater contrasts (mean, 0.41 ± 0.09).

Conclusions: While the group-level results were in precise agreement with the recommendations, semantic-variant primary-progressive aphasia was the only subtype for which the proposed recommendations were both sensitive and specific at an individual level.

MeSH terms

Aged
Aphasia, Primary Progressive / diagnostic imaging*
Brain / diagnostic imaging*
Cohort Studies
Female
Humans
Magnetic Resonance Imaging / methods*
Male
Middle Aged
Neuroimaging / methods*
Sensitivity and Specificity