Publication:
Can we clinically diagnose dementia with Lewy bodies yet?

dc.contributor.author Halliday, Glenda en_US
dc.contributor.author Huang, Yue en_US
dc.date.accessioned 2021-11-25T12:28:37Z
dc.date.available 2021-11-25T12:28:37Z
dc.date.issued 2013 en_US
dc.description.abstract Dementia with Lewy Bodies (DLB) was initially identified and confirmed primarily by pathology, but is soon to be incorporated into the Diagnostic and Statistical Manual criteria as a clinical disease entity. Despite these advances over more than 20 years, current data suggest that the sensitivity of accurate clinical diagnosis of DLB is still very low, although there is mounting evidence that supportive features may increase diagnostic accuracy. Although DLB remains easy to identify pathologically with different cellular pathologies differentiating it from other dementia syndromes, pathological identification using only Lewy body pathology has been shown to be inaccurate due to overlap with patients without dementia symptoms. A number of studies now suggest that a combination of cellular pathologies, which include α-synuclein and β-amyloid deposition as well as dopamine denervation, assist with differentiating this dementia syndrome from others. The clinical and pathological overlap with the tauopathy of Alzheimer’s disease still remains to be clarified. To determine more robust and independent clinicopathological correlates from Alzheimer’s disease, longitudinal prospective studies, using specific clinical batteries on dementia patients reaching the proposed criteria for DLB, with post-mortem assessment of the multiple pathologies associated with dementia, are required. Identifying genetic causes for DLB is another approach to investigate the pathogenesis of DLB. However this approach has been hindered to date by difficulties with identifying DLB clinically. The use of novel techniques is likely to advance knowledge on the pathogenesis of DLB and assist with redefining clinical and pathologic diagnostic criteria. To achieve the goal of more accurate clinical diagnosis of DLB, breakthroughs are necessary on the pathogenesis of DLB. en_US
dc.identifier.uri http://hdl.handle.net/1959.4/53321
dc.language English
dc.language.iso EN en_US
dc.rights CC BY-NC-ND 3.0 en_US
dc.rights.uri https://creativecommons.org/licenses/by-nc-nd/3.0/au/ en_US
dc.source Legacy MARC en_US
dc.subject.other Genetics en_US
dc.subject.other Dementia with Lewy bodies en_US
dc.subject.other Diagnosis en_US
dc.subject.other Pathogenesis en_US
dc.subject.other Pathology en_US
dc.title Can we clinically diagnose dementia with Lewy bodies yet? en_US
dc.type Journal Article en
dcterms.accessRights open access
dspace.entity.type Publication en_US
unsw.accessRights.uri https://purl.org/coar/access_right/c_abf2
unsw.identifier.doiPublisher http://dx.doi.org/10.1186/2047-9158-2-4 en_US
unsw.relation.FunderRefNo GNT0630434 en_US
unsw.relation.faculty Medicine & Health
unsw.relation.fundingScheme Uncoupled Research Fellowship en_US
unsw.relation.ispartofissue 4 en_US
unsw.relation.ispartofjournal Translational Neurodegeneration en_US
unsw.relation.ispartofpagefrompageto 1-9 en_US
unsw.relation.ispartofvolume 2 en_US
unsw.relation.originalPublicationAffiliation Halliday, Glenda, Neuroscience Research Australia, Faculty of Medicine, UNSW en_US
unsw.relation.originalPublicationAffiliation Huang, Yue, Neuroscience Research Australia, Faculty of Medicine, UNSW en_US
unsw.relation.school Neuroscience Research Australia *
unsw.subject.fieldofresearchcode 110903 Central Nervous System en_US
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