Diagnostic Validation for Participants in the Washington State Parkinson Disease Registry

Kim, Hojoong M.; Leverenz, James B.; Burdick, Daniel; Srivatsal, Sindhu; Pate, Jennifer E.; Hu, Shu‐Ching; Millard, Steven P.; Davis, Marie Y.; Samii, Ali; Zabetian, Cyrus P.

doi:10.1155/2018/3719578

Cited by 20 publications

(21 citation statements)

References 15 publications

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“…Overall, in our study, self-report of physician diagnosis of PD alone, while agreeing reasonably well with diagnostic criteria, did not perform as well, as reported in some prior studies [9][10][11]. Lower performance of PD self-report in our current effort than in FAME may be because FAME used in-person clinical assessment while we relied on self-reports of symptoms for diagnosis and included symptoms information provided by proxies which themselves could be subject to misclassification.…”

Section: Discussionsupporting

confidence: 45%

“…Likewise, in the Women’s Health and Aging Study I, the agreement between self-report of physician diagnosis of PD and medical record was also very high (sensitivity: 89%; specificity, positive predictive value, and negative predictive value:100%) [ 9 ]. Another study, that employed in-person examination, medical records, or data from prior research to validate PD in participants (recruited based on self-report of physician diagnosis of PD) in the Washington State Parkinson Disease Registry, found that 93.4% of the registry participants met the UK Biobank criteria for PD [ 10 ]. Lastly, in the FAME study, 84% of self-reports were confirmed by clinical diagnostic criteria [ 14 ].…”

Section: Discussionmentioning

confidence: 99%

“…Although secondary data sources such as medication inventories, medical records, and administrative data, have been used for PD ascertainment in epidemiological studies [2][3][4][5][6][7][8], in large population-based cohorts, researchers often must rely on self-reported physician-made diagnosis, with or without additional clinical information. Few studies have evaluated strategies to optimize self-report for PD case ascertainment in large cohorts [6,[9][10][11], and none specifically in the context of rural farming populations.…”

Section: Introductionmentioning

confidence: 99%

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Parkinson’s disease case ascertainment in a large prospective cohort

et al. 2021

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Background In epidemiologic studies where physician-based case adjudication is not feasible, Parkinson’s disease (PD) case ascertainment is often limited to self-reports which may not be accurate. We evaluated strategies to identify PD cases in the Agricultural Health Study (AHS). Methods Doctor-diagnosed PD was self-reported on all cohort-wide surveys; potential cases were also identified from death certificates. Follow-up surveys asked about PD-related motor and non-motor symptoms. For PD confirmation, we collected additional diagnosis, symptom, and treatment data from 510 potential PD cases or their proxy (65% of those contacted) in a supplemental screener and obtained medical records for a subset (n = 65). We classified PD cases using established criteria and screener data. Results Of 510 potential PD cases, 75% were considered “probable” or “possible”; this proportion increased among participants diagnosed by a specialist (81.2%), taking PD medication (85.2%), or reporting ≥5 motor symptoms (86.8%) in a regular AHS survey. Of those with medical records, 93% (57 of 61) of probable or possible PD was confirmed. Never-smoking and non-motor and motor symptoms reported in prior AHS surveys were more common with probable/possible PD than unconfirmed PD. Conclusion In this retrospective PD case ascertainment effort, we found that PD self-report with information on motor symptoms or medications may be a reasonable alternative for identifying PD cases when physician exam is not feasible. Because of intervening mortality, screeners could not be obtained from about one-third of those contacted. Thus, findings warrant replication.

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Section: Discussionsupporting

confidence: 45%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Parkinson’s disease case ascertainment in a large prospective cohort

et al. 2021

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“…However, studies have shown that the accuracy of self-reported PD in this context is high. 12 The NMS-Quest assesses the presence of diplopia but not its frequency or severity, which limits our ability to determine the extent to which diplopia is clinically significant and contributes directly to reduced quality of life. Finally, we were unable to distinguish between monocular and binocular diplopia, and while self-reported diplopia has been shown to correlate highly with quantitative examination-based measures of ocular misalignment, 13,14 this has not been validated in the context of the NMS-Quest in PD, so it is possible for blurry vision or other visual symptoms to be confused for diplopia.…”

Section: Discussionmentioning

confidence: 99%

“…Additionally, participants are not assessed in person to confirm the diagnosis of PD, as this is a large‐scale electronic survey. However, studies have shown that the accuracy of self‐reported PD in this context is high 12 . The NMS‐Quest assesses the presence of diplopia but not its frequency or severity, which limits our ability to determine the extent to which diplopia is clinically significant and contributes directly to reduced quality of life.…”

Section: Discussionmentioning

confidence: 99%

Prevalence and Risk Factors for Double Vision in Parkinson Disease

Hamedani

Maguire

Marras

et al. 2021

Movement Disord Clin Pract

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BackgroundBackground: Some patients with Parkinson Disease (PD) report double vision, but its prevalence and determinants are unknown. Objectives Objectives: To determine the prevalence and risk factors for diplopia in PD. Methods Methods: Using data from 26,790 PD patients and 9257 controls in the Fox Insight Study, we compared the prevalence of diplopia using the Non-Movement Symptom Questionnaire. Associations with age, race, gender, disease duration, and scores on MDS-UPDRS part II, and Penn Parkinson's Daily Activity Questionnaire were assessed with generalized estimating equations. ResultsResults: The point prevalence of diplopia was higher in PD (18.1%) than controls (6.3%, P < 0.001) at baseline, and 28.2% of all PD patients reported diplopia at least once during the study (period prevalence). PD patients with diplopia were more likely to be older, non-white, have greater disease duration, and report greater motor, non-motor, and daily activity limitations. Conclusions Conclusions: Diplopia is common and associates with motor and non-motor severity in PD.Visual dysfunction is a non-motor symptom of Parkinson disease (PD). 1 One of the most common and distressing visual symptoms of PD is double vision, which is caused by convergence insufficiency and other patterns of acquired strabismus and has been postulated to reflect brainstem PD pathology affecting supranuclear gaze-holding structures. 2 However, the prevalence of diplopia in PD is unknown. Studies have reported diplopia in anywhere from 10% to 30% of PD patients, 1,3-8 but these wideranging estimates are based on small studies of patients recruited from tertiary movement disorders or neuro-ophthalmology clinics, which may be biased towards greater disease severity and are likely not reflective of the general PD population. Clinicbased cohorts are also prone to under-ascertainment, as neurologists may not be comfortable addressing visual symptoms, and patients frequently do not disclose non-motor symptoms such as double vision unless specifically asked. 9 As diplopia can also occur in individuals without PD, it is also unclear whether the prevalence of diplopia in PD is greater than expected for age and other comorbidities or whether the increased burden is an artifact of increased health care utilization. Because diplopia is easily treatable with prisms, characterizing the burden and risk factors in PD is essential for developing screening and treatment guidelines. In this study, we examine the prevalence and risk factors for diplopia in a longitudinal survey of more than 25,000 PD patients.

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Constricting Life Space and Likelihood of Neurodegenerative Disease in Community-Dwelling Older Men

Bock,

Hoang,

Cawthon

et al. 2023

JAMA Netw Open

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ImportanceLife space is a measure of the frequency, range, and independence of movement through the environment. There is increasing interest in life space as a holistic measure of function in older adults, but the association between change in life space and incident neurodegenerative disease is unknown.ObjectiveTo evaluate the association between change in life space and cognitive decline or incident neurodegenerative disease over 7 years among community-dwelling older men.Design, Setting, and ParticipantsIn this cohort study, logistic regression analyses were used to examine the association of baseline and change in life space with change in cognition unadjusted and adjusted for demographics, cardiovascular risk factors, depression, gait speed, and physical activity. Mixed linear effects models were used to evaluate the association between change in life space and change in cognition. Men were recruited from 6 US sites to participate in a prospective, community-based cohort study of aging and followed-up from 2007 to 2014. Individuals with prevalent dementia or Parkinson disease (PD) at baseline were excluded. Data were analyzed from May 2022 to September 2023.ExposureLife space, assessed using the University of Alabama at Birmingham Life Space Assessment and divided into tertiles.Main Outcomes and MeasuresParticipants completed the Modified Mini-Mental State (3MS) Test, and Trail-Making Test Part B at baseline and 7 years later. At follow-up, participants were asked about a new physician diagnosis of dementia and PD.ResultsA total of 1684 men (mean [SD] age, 77.1 [4.2] years) were recruited and over 7 years of follow-up, 80 men (4.8%) developed dementia and 23 men (1.4%) developed PD. Mean (SD) life space score was 92.9 (18.7) points and mean (SD) change was −9.9 (22.3) points over follow up. In the adjusted model, each 1-SD decrement in life space was associated with increased odds of dementia (odds ratio [OR], 1.59; 95% CI, 1.28-1.98) but not PD (OR, 1.48; 95% CI, 0.97-2.25). For each 1-SD decrement in life space, men worsened by 20.6 (95% CI, 19.8-21.1) seconds in their Trails B score (P &lt; .001) and declined by 1.2 (95% CI, 1.0-1.3) points in their 3MS score (P &lt; .001) over 7 years.Conclusions and RelevanceIn this study of 1684 men followed up over 7 years, change in life space was associated with faster cognitive decline and increased likelihood of neurodegenerative illness. Future studies should examine the role of clinician assessments or wearable electronics in tracking life space in older adults at risk of cognitive decline and neurodegenerative illness.

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Diagnostic Validation for Participants in the Washington State Parkinson Disease Registry

Cited by 20 publications

References 15 publications

Parkinson’s disease case ascertainment in a large prospective cohort

Parkinson’s disease case ascertainment in a large prospective cohort

Prevalence and Risk Factors for Double Vision in Parkinson Disease

Constricting Life Space and Likelihood of Neurodegenerative Disease in Community-Dwelling Older Men

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