Elevated common variant genetic risk for tourette syndrome in a densely-affected pedigree.

Crowley, J.J.

doi:10.1038/s41380-021-01277-w

Titre

Elevated common variant genetic risk for tourette syndrome in a densely-affected pedigree.

Type

article

Institution

UNIL/CHUV/Unisanté + institutions partenaires

Périodique

Molecular Psychiatry

Auteur(s)

Halvorsen, M.

Auteure/Auteur

Szatkiewicz, J.

Auteure/Auteur

Mudgal, P.

Auteure/Auteur

Yu, D.

Auteure/Auteur

Nordsletten, A.E.

Auteure/Auteur

Mataix-Cols, D.

Auteure/Auteur

Mathews, C.A.

Auteure/Auteur

Scharf, J.M.

Auteure/Auteur

Mattheisen, M.

Auteure/Auteur

Robertson, M.M.

Auteure/Auteur

McQuillin, A.

Auteure/Auteur

Crowley, J.J.

Auteure/Auteur

Contributrices/contributeurs

Aschauer, H.

Atzmon, G.

Barr, C.

Barta, C.

Barzilai, N.

Batterson, J.

Berlin, C.

Bodmer, B.

Bohnenpoll, J.

Brown, L.

Bruun, R.

Buckner, R.

Budman, C.

Cath, D.

Cheon, K.A.

Chouinard, S.

Coffey, B.

Coppola, G.

Cox, N.

Crowley, J.

Darrow, S.

Davis, L.

Depienne, C.

Dietrich, A.

Dion, Y.

Elzerman, L.

Fernandez, T.

Freimer, N.

Fremer, C.

Fründt, O.

Garcia-Delgar, B.

Gilbert, D.

Grados, M.

Greenberg, E.

Grice, D.

Hagstrøm, J.

Halvorsen, M.

Hartmann, A.

Hebebrand, J.

Hedderly, T.

Heiman, G.

Heyman, I.

Hinney, A.

Hirschtritt, M.

Hoekstra, P.

Hong, H.

Huang, A.

Huyser, C.

Ibanez-Gomez, L.

Illmann, C.

Jankovic, J.

Kim, Y.

Kim, Y.S.

King, R.

Knowles, J.

Koh, Y.J.

Konstantinidis, A.

Kook, S.

Kuperman, S.

Kurlan, R.

Leckman, J.

Lee, P.

Leventhal, B.

Ludolph, A.

Luðvigsson, P.

Lyon, G.

Madruga-Garrido, M.

Malaty, I.

Maras, A.

Mataix-Cols, D.

Mathews, C.

Mattheisen, M.

McMahon, W.

McQuillin, A.

Mir, P.

Moessner, R.

Morer, A.

Mudgal, P.

Mueller-Vahl, K.

Murphy, T.

Münchau, A.

Nagy, P.

Nawaz, M.

Neale, B.

Nordsletten, A.

Nöthen, M.

Okun, M.

Ophoff, R.

Osiecki, L.

Paschou, P.

Pato, C.

Pato, M.

Pauls, D.

Plessen, K.

Posthuma, D.

Richer, P.

Rizzo, R.

Robertson, M.

Roessner, V.

Roffman, J.

Rouleau, G.

Sandor, P.

Sæmundsen, E.

Scharf, J.

Schlögelhofer, M.

Shin, E.Y.

Singer, H.

Smit, J.

Smoller, J.

Song, D.H.

Song, J.

Stamenkovic, M.

State, M.

Stefansson, H.

Stefansson, K.

Stuhrmann, M.

Sul, J.

Sæmundsen, E.

Szatkiewicz, J.

Tarnok, Z.

Thorarensen, Ó.

Tischfield, J.

Tsetsos, F.

Tübing, J.

Visscher, F.

Wagner, M.

Wanderer, S.

Wang, S.

Willsey, J.

Wolanczyk, T.

Woods, D.

Woods, M.

Worbe, Y.

Yu, D.

Zelaya, I.

Zinner, S.

Groupes de travail

Psychiatric Genomics Consortium TS/OCD Working Group

Liens vers les personnes

Von Plessen, Kerstin Jessica

Liens vers les unités

Direction SUPEA

ISSN

1476-5578

Statut éditorial

Publié

Date de publication

2021-12

Volume

26

Numéro

12

Première page

7522

Dernière page/numéro d’article

7529

Peer-reviewed

Oui

Langue

anglais

Notes

Publication types: Journal Article ; Research Support, N.I.H., Extramural ; Research Support, Non-U.S. Gov't
Publication Status: ppublish

Résumé

Tourette syndrome (TS) is a highly heritable neuropsychiatric disorder with complex patterns of genetic inheritance. Recent genetic findings in TS have highlighted both numerous common variants with small effects and a few rare variants with moderate or large effects. Here we searched for genetic causes of TS in a large, densely-affected British pedigree using a systematic genomic approach. This pedigree spans six generations and includes 122 members, 85 of whom were individually interviewed, and 53 of whom were diagnosed as "cases" (consisting of 28 with definite or probable TS, 20 with chronic multiple tics [CMT], and five with obsessive-compulsive behaviors [OCB]). A total of 66 DNA samples were available (25 TS, 15 CMT, 4 OCB cases, and 22 unaffecteds) and all were genotyped using a dense single nucleotide polymorphism (SNP) array to identify shared segments, copy number variants (CNVs), and to calculate genetic risk scores. Eight cases were also whole genome sequenced to test whether any rare variants were shared identical by descent. While we did not identify any notable CNVs, single nucleotide variants, indels or repeat expansions of near-Mendelian effect, the most distinctive feature of this family proved to be an unusually high load of common risk alleles for TS. We found that cases within this family carried a higher load of TS common variant risk similar to that previously found in unrelated TS cases. Thus far, the strongest evidence from genetic data for contribution to TS risk in this family comes from multiple common risk variants rather than one or a few variants of strong effect.

Sujets

Humans

Pedigree

Polymorphism, Single ...

Risk Factors

Tic Disorders

Tourette Syndrome/gen...

PID Serval

serval:BIB_53E970B13A34

DOI

10.1038/s41380-021-01277-w

PMID

34526668

WOS

000696144100002

Permalien

https://iris.unil.ch/handle/iris/123560

Date de création

2021-11-12T13:57:05.328Z

Date de création dans IRIS

2025-05-20T20:20:41Z

Fichier(s)

Nom

34526668_BIB_53E970B13A34.pdf

Version du manuscrit

postprint

Taille

768.62 KB

Format

Adobe PDF

PID Serval

serval:BIB_53E970B13A34.P001

URN

urn:nbn:ch:serval-BIB_53E970B13A340

Somme de contrôle

(MD5):d52c26c2146f394dfa259fb66d1aac0f