Please use this identifier to cite or link to this item: http://hdl.handle.net/1893/31298
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dc.contributor.authorArgyropoulos, Georgios P Den_UK
dc.contributor.authorMoore, Laurenen_UK
dc.contributor.authorLoane, Clareen_UK
dc.contributor.authorRoca-Fernandez, Adrianaen_UK
dc.contributor.authorLage-Martinez, Carmenen_UK
dc.contributor.authorGurau, Oanaen_UK
dc.contributor.authorIrani, Sarosh Ren_UK
dc.contributor.authorZeman, Adamen_UK
dc.contributor.authorButler, Christopher Ren_UK
dc.date.accessioned2020-06-19T00:02:37Z-
dc.date.available2020-06-19T00:02:37Z-
dc.date.issued2020-03-24en_UK
dc.identifier.urihttp://hdl.handle.net/1893/31298-
dc.description.abstractObjective We investigated the nature and neural foundations of pathologic tearfulness in a uniquely large cohort of patients who had presented with autoimmune limbic encephalitis (aLE). Methods We recruited 38 patients (26 men, 12 women; median age 63.06 years; interquartile range [IQR] 16.06 years) in the postacute phase of aLE who completed questionnaires probing emotion regulation. All patients underwent structural/functional MRI postacutely, along with 67 age- and sex-matched healthy controls (40 men, 27 women; median age 64.70 years; IQR 19.87 years). We investigated correlations of questionnaire scores with demographic, clinical, neuropsychological, and brain imaging data across patients. We also compared patients diagnosed with pathologic tearfulness and those without, along with healthy controls, on gray matter volume, resting-state functional connectivity, and activity. Results Pathologic tearfulness was reported by 50% of the patients, while no patient reported pathologic laughing. It was not associated with depression, impulsiveness, memory impairment, executive dysfunction in the postacute phase, or amygdalar abnormalities in the acute phase. It correlated with changes in specific emotional brain networks: volume reduction in the right anterior hippocampus, left fusiform gyrus, and cerebellum, abnormal hippocampal resting-state functional connectivity with the posteromedial cortex and right middle frontal gyrus, and abnormal hemodynamic activity in the left fusiform gyrus, right inferior parietal lobule, and ventral pons. Conclusions Pathologic tearfulness is common following aLE, is not a manifestation of other neuropsychiatric features, and reflects abnormalities in networks of emotion regulation beyond the acute hippocampal focus. The condition, which may also be present in other neurologic disorders, provides novel insights into the neural basis of affective control and its dysfunction in disease.en_UK
dc.language.isoenen_UK
dc.publisherOvid Technologies (Wolters Kluwer Health)en_UK
dc.relationArgyropoulos GPD, Moore L, Loane C, Roca-Fernandez A, Lage-Martinez C, Gurau O, Irani SR, Zeman A & Butler CR (2020) Pathologic tearfulness after limbic encephalitis: A novel disorder and its neural basis. Neurology, 94 (12), pp. e1320-e1335. https://doi.org/10.1212/wnl.0000000000008934en_UK
dc.rightsThis is an open access article distributed under the terms of the Creative Commons Attribution License 4.0 (CC BY - https://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.en_UK
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/en_UK
dc.subjectClinical Neurologyen_UK
dc.titlePathologic tearfulness after limbic encephalitis: A novel disorder and its neural basisen_UK
dc.typeJournal Articleen_UK
dc.identifier.doi10.1212/wnl.0000000000008934en_UK
dc.identifier.pmid31980582en_UK
dc.citation.jtitleNeurologyen_UK
dc.citation.issn1526-632Xen_UK
dc.citation.issn0028-3878en_UK
dc.citation.volume94en_UK
dc.citation.issue12en_UK
dc.citation.spagee1320en_UK
dc.citation.epagee1335en_UK
dc.citation.publicationstatusPublisheden_UK
dc.citation.peerreviewedRefereeden_UK
dc.type.statusVoR - Version of Recorden_UK
dc.contributor.funderMedical Research Councilen_UK
dc.author.emailgeorgios.argyropoulos@stir.ac.uken_UK
dc.citation.date24/01/2020en_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.contributor.affiliationUniversity of Exeteren_UK
dc.contributor.affiliationUniversity of Oxforden_UK
dc.identifier.isiWOS:000530267800020en_UK
dc.identifier.scopusid2-s2.0-85082342539en_UK
dc.identifier.wtid1629325en_UK
dc.contributor.orcid0000-0001-8267-6861en_UK
dc.contributor.orcid0000-0002-7667-9748en_UK
dc.contributor.orcid0000-0003-4875-658Xen_UK
dc.contributor.orcid0000-0002-7502-9284en_UK
dc.date.accepted2019-10-03en_UK
dcterms.dateAccepted2019-10-03en_UK
dc.date.filedepositdate2020-06-07en_UK
rioxxterms.apcnot requireden_UK
rioxxterms.typeJournal Article/Reviewen_UK
rioxxterms.versionVoRen_UK
local.rioxx.authorArgyropoulos, Georgios P D|0000-0001-8267-6861en_UK
local.rioxx.authorMoore, Lauren|en_UK
local.rioxx.authorLoane, Clare|en_UK
local.rioxx.authorRoca-Fernandez, Adriana|en_UK
local.rioxx.authorLage-Martinez, Carmen|en_UK
local.rioxx.authorGurau, Oana|en_UK
local.rioxx.authorIrani, Sarosh R|0000-0002-7667-9748en_UK
local.rioxx.authorZeman, Adam|0000-0003-4875-658Xen_UK
local.rioxx.authorButler, Christopher R|0000-0002-7502-9284en_UK
local.rioxx.projectProject ID unknown|Medical Research Council|http://dx.doi.org/10.13039/501100000265en_UK
local.rioxx.freetoreaddate2020-06-18en_UK
local.rioxx.licencehttp://creativecommons.org/licenses/by/4.0/|2020-06-18|en_UK
local.rioxx.filenamee1320.full.pdfen_UK
local.rioxx.filecount1en_UK
local.rioxx.source1526-632Xen_UK
Appears in Collections:Psychology Journal Articles

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