Impaired olfaction and other prodromal features in the Parkinson At-Risk Syndrome study
β Scribed by Andrew Siderowf; Danna Jennings; Shirley Eberly; David Oakes; Keith A. Hawkins; Albert Ascherio; Matthew B. Stern; Kenneth Marek; the PARS Investigators
- Book ID
- 102945995
- Publisher
- John Wiley and Sons
- Year
- 2012
- Tongue
- English
- Weight
- 786 KB
- Volume
- 27
- Category
- Article
- ISSN
- 0885-3185
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β¦ Synopsis
Abstract
To test the association between impaired olfaction and other prodromal features of PD in the Parkinson AtβRisk Syndrome Study. The onset of olfactory dysfunction in PD typically precedes motor features, suggesting that olfactory testing could be used as a screening test. A combined strategy that uses other prodromal nonmotor features, along with olfactory testing, may be more efficient than hyposmia alone for detecting the risk of PD. Individuals with no neurological diagnosis completed a mail survey, including the 40βitem University of Pennsylvania Smell Identification Test, and questions on prodromal features of PD. The frequency of reported nonmotor features was compared across individuals with and without hyposmia. A total of 4,999 subjects completed and returned the survey and smell test. Of these, 669 were at or below the 15th percentile based on age and gender, indicating hyposmia. Hyposmics were significantly more likely to endorse nonmotor features, including anxiety and depression, constipation, and rapid eye movement sleep behavior disorder symptoms, and to report changes in motor function. Twentyβsix percent of subjects with combinations of four or more nonmotor features were hyposmic, compared to 12% for those reporting three or fewer nonmotor features (P < 0.0001). Hyposmia is associated with other nonmotor features of PD in undiagnosed individuals. Further assessment of hyposmic subjects using more specific markers for degeneration, such as dopamine transporter imaging, will evaluate whether combining hyposmia and other nonmotor features is useful in assessing the risk of future neurodegeneration. Β© 2012 Movement Disorder Society Β© 2012 Movement Disorder Society
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