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Parkinson’s Families Project: a UK-wide study of early onset and familial Parkinson’s disease

Output Details

The Parkinson’s Families Project is a UK-wide study aimed at identifying genetic variation associated with familial and early-onset Parkinson’s disease (PD). We recruited individuals with a clinical diagnosis of PD and age at motor symptom onset ≤ 45 years and/or a family history of PD in up to third-degree relatives. Where possible, we also recruited affected and unaffected relatives. We analysed DNA samples with a combination of single nucleotide polymorphism (SNP) array genotyping, multiplex ligation-dependent probe amplification (MLPA), and whole-genome sequencing (WGS). We investigated the association between identified pathogenic mutations and demographic and clinical factors such as age at motor symptom onset, family history, motor symptoms (MDS-UPDRS) and cognitive performance (MoCA). We performed baseline genetic analysis in 718 families, of which 205 had sporadic early-onset PD (sEOPD), 113 had familial early-onset PD (fEOPD), and 400 had late-onset familial PD (fLOPD). 69 (9.6%) of these families carried pathogenic variants in known monogenic PD-related genes. The rate of a molecular diagnosis increased to 28.1% in PD with motor onset ≤ 35 years. We identified pathogenic variants in LRRK2 in 4.2% of families, and biallelic pathogenic variants in PRKN in 3.6% of families. We also identified two families with SNCA duplications and three families with a pathogenic repeat expansion in ATXN2, as well as single families with pathogenic variants in VCP, PINK1, PNPLA6, PLA2G6, SPG7, GCH1, and RAB32. An additional 73 (10.2%) families were carriers of at least one pathogenic or risk GBA1 variant. Most early-onset and familial PD cases do not have a known genetic cause, indicating that there are likely to be further monogenic causes for PD.
Tags
  • DNA
  • Early onset PD
  • Familial
  • GBA1
  • Genetics
  • LRRK2
  • Parkinson's disease
  • SNCA
  • SNPs (Single Nucleotide Polymorphisms)
  • United Kingdom (UK)

Meet the Authors

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    Clodagh Towns

    External Collaborator

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    Zih-Hua Fang

    External Collaborator

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    Manuela Tan

    External Collaborator

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    SImona Jasaityte

    External Collaborator

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    Theresa Schmaderer

    External Collaborator

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    Elenaor Stanford

    External Collaborator

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    Miriam I Pollard

    External Collaborator

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    Russel Tilney

    External Collaborator

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    Magan Hodgson

    External Collaborator

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    Lesley Wu

    External Collaborator

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    Robyn Labrum

    External Collaborator

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    Jason Hehir

    External Collaborator

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    James Polke

    External Collaborator

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    Lara M Lange

    External Collaborator

  • Anthony Schapira, PhD

    Lead PI (Core Leadership): Team Schapira

    University College London

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    Kailash Bhatia

    External Collaborator

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    GP2

    External Collaborator

  • Andrew Singleton, PhD

    Global Parkinson's Genetics Program

  • Cornelis Blauwendraat, PhD

    Coalition for Aligning Science

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    Christine Klein

    External Collaborator

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    Henry Houlden

    External Collaborator

  • Nicholas Wood, PhD

    Lead PI (Core Leadership): Team Wood

    University College London

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    Paul Jarman

    External Collaborator

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    Huw Morris

    External Collaborator

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    Raquel Real

    External Collaborator

Aligning Science Across Parkinson's
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