MSH3 modifies somatic instability and disease severity in Huntington’s and myotonic dystrophy type 1
Author:
Flower Michael1, Lomeikaite Vilija2, Ciosi Marc2, Cumming Sarah2, Morales Fernando23, Lo Kitty4, Hensman Moss Davina1, Jones Lesley5, Holmans Peter5, Monckton Darren G2, Tabrizi Sarah J1, Kraus Peter, Hoffman Rainer, Tobin Alan, Borowsky Beth, Keenan S, Whitlock Kathryn B, Queller Sarah, Campbell Colin, Wang Chiachi, Langbehn Doug, Axelson Eric, Johnson Hans, Acharya Tanka, Cash Dave M, Frost Chris, Jones Rebecca, Jurgens Caroline, ‘t Hart Ellen P, van der Grond Jeroen, Witjes- Ane Marie-Noelle N, Roos Raymund A C, Dumas Eve M, van den Bogaard Simon J A, Stopford Cheryl, Craufurd David, Callaghan Jenny, Arran Natalie, Rosas Diana D, Lee S, Monaco W, O’Regan Alison, Milchman Cassie, Frajman E, Labuschagne Izelle, Stout Julie, Campbell Melissa, Andrews Sophie C, Bechtel Natalie, Reilmann Ralf, Bohlen Stefan, Kennard Chris, Berna Claire, Hicks Stephen, Durr Alexandra, Pourchot C, Bardinet Eric, Nigaud Kevin, Valabre Romain, gue `, Lehericy Stephane, Marelli Cecilia, Jauffret Celine, Justo Damian, Leavitt Blair, Decolongon Joji, Sturrock Aaron, Coleman Alison, Santos Rachelle Dar, Patel A, Gibbard Claire, Whitehead Daisy, Wild Ed, Owen Gail, Crawford Helen, Malone Ian, Lahiri Nayana, Fox Nick C, Hobbs Nicola Z, Scahill Rachael I, Ordidge Roger, Pepple Tracey, Read Joy, Say Miranda J, Landwehrmeyer Bernhard, Daidj Ferroudja, Bassez Guillaume, Lignier Baptiste, Couppey Florence, Delmas Stéphanie, Deux Jean-François, Hankiewicz Karolina, Dogan Celine, Minier Lisa, Chevalier Pascale, Hamadouche Amira, Catt Michael, van Hees Vincent, Catt Sharon, Schwalber Ameli, Dittrich Juliane, Kierkegaard Marie, Wenninger Stephan, Schoser Benedikt, Schüller Angela, Stahl Kristina, Künzel Heike, Wolff Martin, Jellinek Anna, Moreno Cecilia Jimenez, Gorman Grainne, Lochmüller Hanns, Trenell Michael, van Laar Sandra, Wood Libby, Cassidy Sophie, Newman Jane, Charman Sarah, Steffaneti Renae, Taylor Louise, Brownrigg Allan, Day Sharon, Atalaia Antonio, Raaphorst Joost, Okkersen Kees, van Engelen Baziel, Nikolaus Stephanie, Cornelissen Yvonne, van Nimwegen Marlies, Maas Daphne, Klerks Ellen, Bouman Sacha, Knoop Hans, Heskamp Linda, Heerschap Arend, Rahmadi Ridho, Groot Perry, Heskes Tom, Kapusta Katarzyna, Glennon Jeffrey, Abghari Shaghayegh, Aschrafi Armaz, Poelmans Geert, Treweek Shaun, Hogarth Fiona, Littleford Roberta, Donnan Peter, Hapca Adrian, Hannah Michael, McKenzie Emma, Rauchhaus Petra, Cumming Sarah A, Monckton Darren GORCID, Adam Berit, Faber Catharina, Merkies Ingemar, ,
Affiliation:
1. Department of Neurodegenerative Disease and Dementia Research Institute, UCL, UK 2. Institute of Molecular, Cell and Systems Biology, University of Glasgow, UK 3. Instituto de Investigaciones en Salud (INISA), Universidad de Costa Rica, San José, Costa Rica 4. School of Mathematics and Statistics, University of Sydney, Australia 5. MRC Centre for Neuropsychiatric Genetics and Genomics, Cardiff University, UK
Abstract
Abstract
The mismatch repair gene MSH3 has been implicated as a genetic modifier of the CAG·CTG repeat expansion disorders Huntington’s disease and myotonic dystrophy type 1. A recent Huntington’s disease genome-wide association study found rs557874766, an imputed single nucleotide polymorphism located within a polymorphic 9 bp tandem repeat in MSH3/DHFR, as the variant most significantly associated with progression in Huntington’s disease. Using Illumina sequencing in Huntington’s disease and myotonic dystrophy type 1 subjects, we show that rs557874766 is an alignment artefact, the minor allele for which corresponds to a three-repeat allele in MSH3 exon 1 that is associated with a reduced rate of somatic CAG·CTG expansion (P = 0.004) and delayed disease onset (P = 0.003) in both Huntington’s disease and myotonic dystrophy type 1, and slower progression (P = 3.86 × 10−7) in Huntington’s disease. RNA-Seq of whole blood in the Huntington’s disease subjects found that repeat variants are associated with MSH3 and DHFR expression. A transcriptome-wide association study in the Huntington’s disease cohort found increased MSH3 and DHFR expression are associated with disease progression. These results suggest that variation in the MSH3 exon 1 repeat region influences somatic expansion and disease phenotype in Huntington’s disease and myotonic dystrophy type 1, and suggests a common DNA repair mechanism operates in both repeat expansion diseases.
Funder
UK Dementia Research Institute European Union, Medical Research Council
Publisher
Oxford University Press (OUP)
Subject
Clinical Neurology
Cited by
123 articles.
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