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dc.contributor.authorMontembeault, Maxime
dc.contributor.authorBrambati, Simona Maria
dc.contributor.authorLamari, Foudil
dc.contributor.authorMichon, Agnès
dc.contributor.authorSamri, Dalila
dc.contributor.authorEpelbaum, Stéphane
dc.contributor.authorLacomblez, Lucette
dc.contributor.authorLehéricy, Stéphane
dc.contributor.authorHabert, Marie-Odile
dc.contributor.authorDubois, Bruno
dc.contributor.authorKas, Aurélie
dc.contributor.authorMigliaccio, Raffaella
dc.date.accessioned2019-05-24T15:39:59Z
dc.date.availableNO_RESTRICTIONfr
dc.date.available2019-05-24T15:39:59Z
dc.date.issued2018-10-10
dc.identifier.urihttp://hdl.handle.net/1866/21942
dc.publisherElsevierfr
dc.rightsCe document est mis à disposition selon les termes de la Licence Creative Commons Paternité 4.0 International. / This work is licensed under a Creative Commons Attribution 4.0 International License.
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectPosterior cortical atrophyfr
dc.subjectAlzheimer's diseasefr
dc.subjectCerebrospinal fluidfr
dc.subjectBiomarkersfr
dc.subjectGray matter atrophyfr
dc.subjectBrain metabolismfr
dc.subjectNeuropsychologyfr
dc.subjectAtypical dementiafr
dc.subject¹⁸F-FDG PETfr
dc.subjectVoxel-based morphometryfr
dc.titleAtrophy, metabolism and cognition in posterior cortical atrophy spectrum based on AD CSF biomarkersfr
dc.typeArticlefr
dc.contributor.affiliationUniversité de Montréal. Faculté des arts et des sciences. Département de psychologiefr
dc.identifier.doi10.1016/j.nicl.2018.10.010
dcterms.abstractIntroduction In vivo clinical, anatomical and metabolic differences between posterior cortical atrophy (PCA) patients presenting with different Alzheimer's disease (AD) cerebrospinal fluid (CSF) biomarkers profiles are still unknown. Methods Twenty-seven PCA patients underwent CSF examination and were classified as 1) PCA with a typical CSF AD profile (PCA-tAD; abnormal amyloid and T-tau/P-tau biomarkers, n = 13); 2) PCA with an atypical AD CSF profile (PCA-aAD; abnormal amyloid biomarker only, n = 9); and 3) PCA not associated with AD (PCA-nonAD; normal biomarkers, n = 5). All patients underwent clinical and cognitive assessment, structural MRI, and a subset of them underwent brain 18F-FDG PET. Results All patients' groups showed a common pattern of posterior GM atrophy and hypometabolism typical of PCA, as well as equivalent demographics and clinical/cognitive profiles. PCA-tAD patients showed a group-specific pattern of hypometabolism in the left fusiform gyrus and inferior temporal gyrus. PCA-aAD did not present a group-specific atrophy pattern. Finally, group-specific gray matter atrophy in the right dorsolateral prefrontal cortex, left caudate nucleus and right medial temporal regions and hypometabolism in the right supplementary motor area and paracentral lobule were observed in PCA-nonAD patients. Conclusion Our findings suggest that both PCA-tAD and PCA-aAD patients are on the AD continuum, in agreement with the recently suggested A/T/N model. Furthermore, in PCA, the underlying pathology has an impact at least on the anatomo-functional presentation. Brain damage observed in PCA-tAD and PCA-aAD was mostly consistent with the well-described presentation of the disease, although it was more widespread in PCA-tAD group, especially in the left temporal lobe. Additional fronto-temporal (especially dorsolateral prefrontal) damage seems to be a clue to underlying non-AD pathology in PCA, which warrants the need for longitudinal follow-ups to investigate frontal symptoms in these patients.fr
dcterms.isPartOfurn:ISSN:1053-8119fr
dcterms.isPartOfurn:ISSN:1095-9572fr
dcterms.languageengfr
UdeM.ReferenceFournieParDeposantMontembeault M*, Brambati SM, Lamari F, Gallea C, Michon A, Samri D, Epelbaum S, Lacomblez L, Habert MO, Dubois B, Kas A, Migliaccio R. Atrophy, metabolism and cognition in posterior cortical atrophy spectrum based on AD CSF biomarkers. Neuroimage Clin. 2018;20:1018-1025. doi: 10.1016/j.nicl.2018.10.010fr
UdeM.VersionRioxxVersion publiée / Version of Recordfr
oaire.citationTitleNeurolmage
oaire.citationVolume20
oaire.citationStartPage1018
oaire.citationEndPage1025


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Ce document est mis à disposition selon les termes de la Licence Creative Commons Paternité 4.0 International. / This work is licensed under a Creative Commons Attribution 4.0 International License.
Usage rights : Ce document est mis à disposition selon les termes de la Licence Creative Commons Paternité 4.0 International. / This work is licensed under a Creative Commons Attribution 4.0 International License.