Please use this identifier to cite or link to this item: https://repository.monashhealth.org/monashhealthjspui/handle/1/30039
Conference/Presentation Title: Dorsolateral prefrontal activation in Huntington's disease is sensitive to a range of cognitive and behavioral deficits: Cross sectional data from Image-HD.
Authors: Churchyard A.;Georgiou-Karistianis N. ;Ando A.;Chua P.;Stout J.;Gray M.A.;Egan G.;Langmaid R.;Dominguez J.
Institution: (Gray, Egan, Langmaid, Dominguez, Ando, Chua, Stout, Georgiou-Karistianis) School of Psychology and Psychiatry, Faculty of Medicine Nursing and Health Scienc, Monash University, Clayton, VIC, Australia (Egan, Ando) Howard Florey Institute, Florey Neuroscience Institutes, Parkville, VIC, Australia (Egan) Centre for Neuroscience, University of Melbourne, Parkville, VIC, Australia (Egan) Monash Biomedical Imaging (MBI), Monash University, Clayton, VIC, Australia (Churchyard) Department of Neurology, Monash Medical Centre, Clayton, VIC, Australia
Presentation/Conference Date: 24-Oct-2011
Copyright year: 2011
Publisher: Blackwell Publishing Ltd
Publication information: Clinical Genetics. Conference: 2011 World Congress on Huntington's Disease. Melbourne, VIC Australia. Conference Publication: (var.pagings). 80 (SUPPL. 1) (pp 49), 2011. Date of Publication: September 2011.
Abstract: Introduction: Functional integrity of cortico-striatal circuits underlying generalised executive functioning may be compromised by basal ganglia (BG) degeneration during Huntington's Disease (HD). We challenged cortico-striatal function with a shifting response set (SRS) task, and examined associations between the degree of induced neural responses and difficulties with cognition and emotions within HD. Method(s): Thirty-five healthy, 35 matched pre-symptomatic HD (pre-HD) and 30 symptomatic HD (symp-HD) participants completed a computerised SRS task during functional brain scanning (fMRI) at 3 tesla. A 70% performance threshold allowed confident identification of neural activity underpinning SRS (33 control, 32 pre-HD, 20 symp-HD), while associations between neural SRS responses and cognitive-emotional disturbance within the total sample allowed inclusion of dysfunctional responses. Result(s): SRS activated dorsolateral pre-frontal (DLPFC) and cingulate, pre-motor, parietal, and BG regions and deactivated ventromedial pre-frontal cortex (VMPFC). Symp-HD showed greater activation of DLPFC, dorsal cingulate and left anterior insula, and greater deactivation of VMPFC relative to controls, with pre-HD showing similar although less widespread differences relative to controls. Importantly, within symp-HD measures of cognitive and emotional disturbance correlated negatively with DLPFC and dorsal ACC responses, and positively with ventromedial PFC responses evoked during SRS challenge. Conclusion(s): Our findings support previous observations of the contribution of DLPFC, ACC and BG to SRS and indicate that similar behavioural performance in HD requires additional activity within these regions. Critically, our findings suggest that capacity to increase functional brain responses during the transition from pre-HD to symp-HD may be protective against neurocognitive dysfunction.
Conference Start Date: 2011-09-11
Conference End Date: 2011-09-14
DOI: http://monash.idm.oclc.org/login?url=http://dx.doi.org/10.1111/j.1399-0004.2011.01737.x
ISSN: 0009-9163
URI: https://repository.monashhealth.org/monashhealthjspui/handle/1/30039
Type: Conference Abstract
Subjects: emotion
emotional disorder
*Huntington chorea
manager
insula
degeneration
brain
basal ganglion
nerve potential
cognition
functional magnetic resonance imaging
human
brain scintiscanning
frontal cortex
functional magnetic resonance imaging
*Huntington chorea
emotional disorder
emotion
human
brain scintiscanning
frontal cortex
manager
insula
degeneration
brain
basal ganglion
nerve potential
cognition
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