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          Abstract

          Objectives

          To evaluate the proportion of Parkinson's disease (PD) patients identified as having advanced Parkinson's disease (APD) according to physician's judgement in Australia.

          Methods

          This cross-sectional, non-interventional observational study was performed in movement disorder clinics from 18 countries. Results from Australia are presented. Participants included consecutive adults with PD attending routine clinical visits, or inpatients, who could speak English. The primary outcome was the proportion of patients diagnosed with APD via physician judgement.

          Results

          100 patients were recruited in Australia: 61.0% (95% CI 51.4–70.6%) diagnosed with APD by physician judgement. Patients were 66.6 ± 8.5 years, 65% were male, were living at home (97%), and diagnosed with PD for median 10.7 years (0–30.5 years). Motor fluctuations were present in 68%. For those with APD, referral was predominantly to enable access to device assisted therapies (DAT) (49%), while for non-APD, referral was largely for diagnostic purposes (41%). Patients had a median follow-up at the movement disorder clinic of 4.8 years for those with APD, or 3.6 years for non-APD. While 62% were eligible for DAT, only two-thirds of these received them. The most commonly used DAT was deep brain stimulation (64.3%). There was fair agreement between physician's judgement and the APD criteria by Delphi method (Cohen's kappa) 0.325 (95% CI 0.150–0.500) in the Australian subset.

          Conclusions

          The definition of APD requires refinement in order to facilitate greater agreement among movement disorder specialists. A third of APD patients eligible for DAT remain untreated. Better referral and education of patients with APD is needed.

          • The definition of advanced Parkinson's disease requires refinement.

          • Device assisted therapy is recommended in advanced Parkinson's disease.

          • A third of eligible patients are not receiving device assisted therapy.

          • Better referral and education of advanced Parkinson's disease patients is needed.

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          Most cited references25

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          Index for rating diagnostic tests

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            The prevalence of Parkinson's disease: a systematic review and meta-analysis.

            Parkinson's Disease (PD) is a common neurodegenerative disorder. We sought to synthesize studies on the prevalence of PD to obtain an overall view of how the prevalence of this disease varies by age, by sex, and by geographic location. We searched MEDLINE and EMBASE for epidemiological studies of PD from 1985 to 2010. Data were analyzed by age group, geographic location, and sex. Geographic location was stratified by the following groups: 1) Asia, 2) Africa, 3) South America, and 4) Europe/North America/Australia. Meta-regression was used to determine whether a significant difference was present between groups. Forty-seven studies were included in the analysis. Meta-analysis of the worldwide data showed a rising prevalence of PD with age (all per 100,000): 41 in 40 to 49 years; 107 in 50 to 59 years; 173 in 55 to 64 years; 428 in 60 to 69 years; 425 in 65 to 74 years; 1087 in 70 to 79 years; and 1903 in older than age 80. A significant difference was seen in prevalence by geographic location only for individuals 70 to 79 years old, with a prevalence of 1,601 in individuals from North America, Europe, and Australia, compared with 646 in individuals from Asia (P < 0.05). A significant difference in prevalence by sex was found only for individuals 50 to 59 years old, with a prevalence of 41 in females and 134 in males (P < 0.05). PD prevalence increases steadily with age. Some differences in prevalence by geographic location and sex can be detected. © 2014 International Parkinson and Movement Disorder Society.
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              Levodopa-induced dyskinesias.

              Levodopa-induced dyskinesias (LID) are common and difficult to treat. This review focuses on three issues related to LID: clinical features, classification and rating, pathophysiology and pathogenesis, and management. The three primary clinical syndromes are OFF-period dystonia, peak-dose dyskinesia, and diphasic dyskinesia. Several other forms also occur, making the evaluation and choice of treatment complicated. A core component of the pathophysiology of LID is overactivity of the direct striatal output pathway. This pathway provides a direct GABAergic connection by which the striatum inhibits the output regions of the basal ganglia, i.e., the internal globus pallidus and the substantia nigra pars reticulata. Altering dopaminergic dosing and timing can abate dyskinesias, but usually impact the control of parkinsonism. Putative therapies to reduce the problem of dyskinesias could focus on the glutamatergic, GABAergic, alpha2 adrenergic, serotonergic (5HT1A, 5HT2A), opioid, histamine H3, adenosine A2A receptors, the monoamine transport or cannabinoid CB1 receptors systems. The only currently available drug with an evidence-based recommendation on efficacy for dyskinesia is amantadine. Therapy goals include the prevention of dyskinesia and treatment of dyskinesias that are troublesome clinically. New rating measures to assess severity and disability related to dyskinesia are in the process of development and clinimetric testing. Copyright 2007 Movement Disorder Society
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                Author and article information

                Contributors
                Journal
                Clin Park Relat Disord
                Clin Park Relat Disord
                Clinical Parkinsonism & Related Disorders
                Elsevier
                2590-1125
                17 October 2020
                2021
                17 October 2020
                : 4
                : 100075
                Affiliations
                [a ]Movement Disorders Program, Royal Melbourne Hospital, Australia
                [b ]Movement Disorders Unit, Department of Neurology, Westmead Hospital, Australia
                [c ]Sydney Medical School, University of Sydney, Australia
                [d ]UQ Centre for Clinical Research, The University of Queensland, Australia
                [e ]Senior Visiting Neurologist Royal Brisbane & Women's Hospital, Australia
                [f ]Movement Disorders Clinic, Perron Institute, Australia
                [g ]Department of Neurology, Townsville Hospital, Australia
                [h ]Van Cleef Roet Centre for Nervous Diseases, Australia
                [i ]Therapeutic Area Lead, AbbVie, United States of America
                [j ]Study Designated Physician, AbbVie, United States of America
                Author notes
                [* ]Corresponding author at: Movement Disorders Program, The Royal Melbourne Hospital, 300 Grattan Street, Parkville, VIC 3050, Australia. Andrew.Evans@ 123456mh.org.au
                Article
                S2590-1125(20)30043-8 100075
                10.1016/j.prdoa.2020.100075
                8299979
                34316660
                82b92c8c-c744-419d-8655-8d432f1538c6
                © 2020 Published by Elsevier Ltd.

                This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

                History
                : 14 September 2020
                : 13 October 2020
                Categories
                Original Article

                parkinson's disease,diagnosis,advanced parkinson's disease,device assisted therapy

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