Proxy-analysis of the genetics of cognitive decline in Parkinson’s disease through polygenic scores

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作者
Johann Faouzi
Manuela Tan
Fanny Casse
Suzanne Lesage
Christelle Tesson
Alexis Brice
Graziella Mangone
Louise-Laure Mariani
Hirotaka Iwaki
Olivier Colliot
Lasse Pihlstrøm
Jean-Christophe Corvol
机构
[1] AP-HP,Sorbonne Université, Institut du Cerveau–Paris Brain Institute
[2] Hôpital de la Pitié Salpêtrière,ICM, CNRS, Inria, Inserm
[3] CREST–UMR 9194,Univ Rennes, Ensai, CNRS
[4] Oslo University Hospital,Department of Neurology
[5] Inserm,Sorbonne Université, Institut du Cerveau–Paris Brain Institute
[6] AP-HP,ICM, CNRS
[7] Hôpital de la Pitié Salpêtrière,Department of Neurology, Movement Disorder Division
[8] Sorbonne Université,Laboratory of Neurogenetics, National Institute on Aging
[9] Institut du Cerveau–Paris Brain Institute-ICM,Center for Alzheimer’s and Related Dementias (CARD), National Institute on Aging and National Institute of Neurological Disorders and Stroke
[10] CNRS,undefined
[11] Inserm,undefined
[12] AP-HP,undefined
[13] Hôpital de la Pitié Salpêtrière,undefined
[14] DMU Neurosciences,undefined
[15] Département de Génétique,undefined
[16] Sorbonne Université,undefined
[17] Institut du Cerveau–Paris Brain Institute-ICM,undefined
[18] CNRS,undefined
[19] Inserm,undefined
[20] AP-HP,undefined
[21] Hôpital de la Pitié Salpêtrière,undefined
[22] DMU Neurosciences,undefined
[23] Département de Neurologie,undefined
[24] Rush University Medical Center,undefined
[25] National Institutes of Health,undefined
[26] National Institutes of Health,undefined
[27] Data Tecnica International LLC,undefined
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摘要
Cognitive decline is common in Parkinson’s disease (PD) and its genetic risk factors are not well known to date, besides variants in the GBA and APOE genes. However, variation in complex traits is caused by numerous variants and is usually studied with genome-wide association studies (GWAS), requiring a large sample size, which is difficult to achieve for outcome measures in PD. Taking an alternative approach, we computed 100 polygenic scores (PGS) related to cognitive, dementia, stroke, and brain anatomical phenotypes and investigated their association with cognitive decline in six longitudinal cohorts. The analysis was adjusted for age, sex, genetic ancestry, follow-up duration, GBA and APOE status. Then, we meta-analyzed five of these cohorts, comprising a total of 1702 PD participants with 6156 visits, using the Montreal Cognitive Assessment as a cognitive outcome measure. After correction for multiple comparisons, we found four PGS significantly associated with cognitive decline: intelligence (p = 5.26e–13), cognitive performance (p = 1.46e–12), educational attainment (p = 8.52e–10), and reasoning (p = 3.58e–5). Survival analyses highlighted an offset of several years between the first and last quartiles of PGS, with significant differences for the PGS of cognitive performance (5 years) and educational attainment (7 years). In conclusion, we found four PGS associated with cognitive decline in PD, all associated with general cognitive phenotypes. This study highlights the common genetic factors between cognitive decline in PD and the general population, and the importance of the participant’s cognitive reserve for cognitive outcome in PD.
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