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Dive into the research topics where Sarah Duff-Canning is active.

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Featured researches published by Sarah Duff-Canning.


Neurology | 2006

Prospective prevalence of pathologic gambling and medication association in Parkinson disease

Valerie Voon; K. Hassan; Mateusz Zurowski; Sarah Duff-Canning; M. de Souza; Susan H. Fox; Anthony E. Lang; Janis Miyasaki

The authors prospectively screened 297 patients with Parkinson disease (PD), who attended a tertiary clinic, using a modified South Oaks Gambling Scale. Lifetime prevalence of pathologic gambling (PG) was 3.4% and on any dopamine agonist was 7.2%. PG was associated with earlier PD onset and with dopamine agonists but not with agonist subtype or doses. We found no association with a potent D3 receptor agonist.


Movement Disorders | 2008

A comparison of the mini mental state exam to the Montreal cognitive assessment in identifying cognitive deficits in Parkinson's disease.

Cindy Zadikoff; Susan H. Fox; David F. Tang-Wai; Teri Thomsen; Rob M. A. de Bie; Pettarusup Wadia; Janis Miyasaki; Sarah Duff-Canning; Anthony E. Lang; Connie Marras

Dementia is an important and increasingly recognized problem in Parkinsons disease (PD). The mini‐mental state examination (MMSE) often fails to detect early cognitive decline. The Montreal cognitive assessment (MoCA) is a brief tool developed to detect mild cognitive impairment that assesses a broader range of domains frequently affected in PD. The scores on the MMSE and the MoCA were compared in 88 patients with PD. A pronounced ceiling effect was observed with the MMSE but not with the MoCA. The range and standard deviation of scores was larger with the MoCA(7–30, 4.26) than with the MMSE(16–30, 2.55). The percentage of subjects scoring below a cutoff of 26/30 (used by others to detect mild cognitive impairment) was higher on the MoCA (32%) than on the MMSE (11%)(P < 0.000002). Compared to the MMSE, the MoCA may be a more sensitive tool to identify early cognitive impairment in PD.


Movement Disorders | 2013

Measuring mild cognitive impairment in patients with Parkinson's disease.

Connie Marras; Melissa J. Armstrong; Christopher Meaney; Susan H. Fox; Brandon Rothberg; William Reginold; David F. Tang-Wai; David J. Gill; Paul J. Eslinger; Cindy Zadikoff; Nancy Kennedy; Fred Marshall; Mark Mapstone; Kelvin L. Chou; Carol Persad; Irene Litvan; Benjamin T. Mast; Adam Gerstenecker; Sandra Weintraub; Sarah Duff-Canning

We examined the frequency of Parkinson disease with mild cognitive impairment (PD‐MCI) and its subtypes and the accuracy of 3 cognitive scales for detecting PD‐MCI using the new criteria for PD‐MCI proposed by the Movement Disorders Society. Nondemented patients with Parkinsons disease completed a clinical visit with the 3 screening tests followed 1 to 3 weeks later by neuropsychological testing. Of 139 patients, 46 met Level 2 Task Force criteria for PD‐MCI when impaired performance was based on comparisons with normative scores. Forty‐two patients (93%) had multi‐domain MCI. At the lowest cutoff levels that provided at least 80% sensitivity, specificity was 44% for the Montreal Cognitive Assessment and 33% for the Scales for Outcomes in Parkinsons Disease‐Cognition. The Mini‐Mental State Examination could not achieve 80% sensitivity at any cutoff score. At the highest cutoff levels that provided specificity of at least 80%, sensitivities were low (≤44%) for all tests. When decline from estimated premorbid levels was considered evidence of cognitive impairment, 110 of 139 patients were classified with PD‐MCI, and 103 (94%) had multi‐domain MCI. We observed dramatic differences in the proportion of patients who had PD‐MCI using the new Level 2 criteria, depending on whether or not decline from premorbid level of intellectual function was considered. Recommendations for methods of operationalizing decline from premorbid levels constitute an unmet need. Among the 3 screening tests examined, none of the instruments provided good combined sensitivity and specificity for PD‐MCI. Other tests recommended by the Task Force Level 1 criteria may represent better choices, and these should be the subject of future research.


Brain | 2014

Combined insular and striatal dopamine dysfunction are associated with executive deficits in Parkinson's disease with mild cognitive impairment.

Leigh Christopher; Connie Marras; Sarah Duff-Canning; Yuko Koshimori; Robert Chen; Isabelle Boileau; Bàrbara Segura; Oury Monchi; Anthony E. Lang; Pablo Rusjan; Sylvain Houle; Antonio P. Strafella

The ability to dynamically use various aspects of cognition is essential to daily function, and reliant on dopaminergic transmission in cortico-striatal circuitry. Our aim was to investigate both striatal and cortical dopaminergic changes in patients with Parkinsons disease with mild cognitive impairment, who represent a vulnerable group for the development of dementia. We hypothesized severe striatal dopamine denervation in the associative (i.e. cognitive) region and cortical D2 receptor abnormalities in the salience and executive networks in Parkinsons disease with mild cognitive impairment compared with cognitively normal patients with Parkinsons disease and healthy control subjects. We used positron emission tomography imaging with dopaminergic ligands (11)C-dihydrotetrabenazine, to investigate striatal dopamine neuron integrity in the associative subdivision and (11)C-FLB 457, to investigate cortical D2 receptor availability in patients with Parkinsons disease (55-80 years of age) with mild cognitive impairment (n = 11), cognitively normal patients with Parkinsons disease (n = 11) and age-matched healthy control subjects (n = 14). Subjects were administered a neuropsychological test battery to assess cognitive status and determine the relationship between dopaminergic changes and cognitive performance. We found that patients with mild cognitive impairment had severe striatal dopamine depletion in the associative (i.e. cognitive) subdivision as well as reduced D2 receptor availability in the bilateral insula, a key cognitive hub, compared to cognitively normal patients and healthy subjects after controlling for age, disease severity and daily dopaminergic medication intake. Associative striatal dopamine depletion was predictive of D2 receptor loss in the insula of patients with Parkinsons disease with mild cognitive impairment, demonstrating interrelated striatal and cortical changes. Insular D2 levels also predicted executive abilities in these patients as measured using a composite executive z-score obtained from neuropsychological testing. Furthermore we assessed cortical thickness to ensure that D2 receptor changes were not confounded by brain atrophy. There was no difference between groups in cortical thickness in the insula, or any other cortical region of interest. These findings suggest that striatal dopamine denervation combined with insular D2 receptor loss underlie mild cognitive impairment in Parkinsons disease and in particular decline in executive function. Furthermore, these findings suggest a crucial and direct role for dopaminergic modulation in the insula in facilitating cognitive function.


BJUI | 2009

Management of decreased bone mineral density in men starting androgen‐deprivation therapy for prostate cancer

Abbas H. Panju; Henriette Breunis; Angela M. Cheung; Marc Leach; Neil Fleshner; Padraig Warde; Sarah Duff-Canning; Murray Krahn; Gary Naglie; Ian F. Tannock; George Tomlinson; Shabbir M.H. Alibhai

To determine whether clinicians discuss bone‐specific side‐effects with patients on androgen‐deprivation therapy (ADT) for prostate cancer, or prescribe lifestyle and pharmacological interventions for low bone mineral density (BMD), as decreased BMD is a common side‐effect of ADT, leading to increased risk of fracture.


Annals of Neurology | 2015

Salience Network and Parahippocampal Dopamine Dysfunction in Memory-Impaired Parkinson Disease

Leigh Christopher; Sarah Duff-Canning; Yuko Koshimori; Bàrbara Segura; Isabelle Boileau; Robert Chen; Anthony E. Lang; Sylvain Houle; Pablo Rusjan; Antonio P. Strafella

Patients with Parkinson disease (PD) and mild cognitive impairment (MCI) are vulnerable to dementia and frequently experience memory deficits. This could be the result of dopamine dysfunction in corticostriatal networks (salience, central executive networks, and striatum) and/or the medial temporal lobe. Our aim was to investigate whether dopamine dysfunction in these regions contributes to memory impairment in PD.


Dementia and Geriatric Cognitive Disorders | 2013

Impact of Mild Cognitive Impairment on Health-Related Quality of Life in Parkinson's Disease

William Reginold; Sarah Duff-Canning; Christopher Meaney; Melissa J. Armstrong; Susan H. Fox; Brandon Rothberg; Cindy Zadikoff; Nancy Kennedy; David J. Gill; Paul J. Eslinger; Fred Marshall; Mark Mapstone; Kelvin L. Chou; Carol Persad; Irene Litvan; Benjamin T. Mast; David F. Tang-Wai; Anthony E. Lang; Connie Marras

Background/Aims: To assess the impact of mild cognitive impairment (MCI) or cognitive decline on health-related quality of life (HR-QOL) in Parkinsons disease (PD). Methods: HR-QOL measured by the Parkinson Disease Quality of Life Questionnaire (PDQ-39), MCI according to Movement Disorder Society Task Force criteria and cognitive decline from premorbid baseline were assessed in non-demented PD patients at 6 movement disorder clinics. Results: Among 137 patients, after adjusting for education, gender, disease duration, and Movement Disorder Society Unified Parkinsons Disease Rating Scale total score, MCI was associated with worse scores within the PDQ-39 dimension of communication (p = 0.008). Subjects were divided into tertiles of cognitive decline from premorbid level. Scores in the dimension of stigma were worst in the second tertile of cognitive decline (p = 0.03). MCI was associated with worse social support scores in the second tertile of cognitive decline (p = 0.008). Conclusion: MCI and cognitive decline from premorbid baseline are associated with reduced HR-QOL in communication, stigma, and social support domains. The cognitive decline from premorbid baseline modifies the association between MCI and HR-QOL in PD and knowing both will allow a better appreciation of difficulties patients face in daily life.


Brain Structure & Function | 2015

Imaging changes associated with cognitive abnormalities in Parkinson’s disease

Yuko Koshimori; Bàrbara Segura; Leigh Christopher; Nancy J. Lobaugh; Sarah Duff-Canning; Romina Mizrahi; Clement Hamani; Anthony E. Lang; Kelly Aminian; Sylvain Houle

The current study investigates both gray and white matter changes in non-demented Parkinson’s disease (PD) patients with varying degrees of mild cognitive deficits and elucidates the relationships between the structural changes and clinical sequelae of PD. Twenty-six PD patients and 15 healthy controls (HCs) were enrolled in the study. Participants underwent T1-weighted and diffusion tensor imaging (DTI) scans. Their cognition was assessed using a neuropsychological battery. Compared with HCs, PD patients showed significant cortical thinning in sensorimotor (left pre- and postcentral gyri) and cognitive (left dorsolateral superior frontal gyrus [DLSFG]) regions. The DLSFG cortical thinning correlated with executive and global cognitive impairment in PD patients. PD patients showed white matter abnormalities as well, primarily in bilateral frontal and temporal regions, which also correlated with executive and global cognitive impairment. These results seem to suggest that both gray and white matter changes in the frontal regions may constitute an early pathological substrate of cognitive impairment of PD providing a sensitive biomarker for brain changes in PD.


Dementia and geriatric cognitive disorders extra | 2012

Roles of Education and IQ in Cognitive Reserve in Parkinson's Disease-Mild Cognitive Impairment

Melissa J. Armstrong; G. Naglie; Sarah Duff-Canning; Christopher Meaney; David J. Gill; Paul J. Eslinger; Cindy Zadikoff; Mark Mapstone; Kelvin L. Chou; Carol Persad; Irene Litvan; Benjamin T. Mast; Susan H. Fox; David F. Tang-Wai; Connie Marras

Background/Aims: The role of cognitive reserve in Parkinson’s disease (PD)-mild cognitive impairment (MCI) is incompletely understood. Methods: The relationships between PD-MCI, years of education, and estimated premorbid IQ were examined in 119 consecutive non-demented PD patients using logistic regression models. Results: Higher education and IQ were associated with reduced odds of PD-MCI in univariate analysis. In multivariable analysis, a higher IQ was associated with a significantly decreased odds of PD-MCI, but education was not. Conclusion: The association of higher IQ and decreased odds of PD-MCI supports a role for cognitive reserve in PD, but further studies are needed to clarify the interaction of IQ and education and the impact of other contributors such as employment and hobbies.


Movement Disorders | 2012

The pill questionnaire in a nondemented Parkinson's disease population

William Reginold; Melissa J. Armstrong; Sarah Duff-Canning; Anthony E. Lang; David F. Tang-Wai; Susan H. Fox; Brandon Rothberg; Cindy Zadikoff; Nancy Kennedy; David J. Gill; Paul J. Eslinger; Mark Mapstone; Kelvin L. Chou; Carol Persad; Irene Litvan; Benjamin T. Mast; Connie Marras

We assessed the Pill Questionnaire as a screen for mild cognitive impairment in nondemented Parkinsons disease patients.

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Connie Marras

Toronto Western Hospital

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Susan H. Fox

University Health Network

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Irene Litvan

University of California

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