TY - JOUR
T1 - Positive association of dopamine D2 receptor polymorphism with bipolar affective disorder in a European Multicenter Association study of affective disorders
AU - Massat, Isabelle
AU - Souery, Daniel
AU - Del-Favero, Jurgen
AU - Van Gestel, Sofie
AU - Serretti, Alessandro
AU - Macciardi, Fabio
AU - Smeraldi, Enrico
AU - Kaneva, Radka
AU - Adolfsson, Rolf
AU - Nylander, Peter O.
AU - Blackwood, Douglas
AU - Muir, Walter
AU - Papadimitriou, George N.
AU - Dikeos, Dimitris
AU - Oru, Lilijana
AU - Segman, Ronnen H.
AU - Ivezi, Sladjana
AU - Aschauer, Harold
AU - Ackenheil, Manfred
AU - Fuchshuber, S.
AU - Dam, Henrik
AU - Jakovljevi, Miro
AU - Peltonen, Leena
AU - Hilger, Christiane
AU - Hentges, François
AU - Staner, Luc
AU - Milanova, Vihra
AU - Jazin, Elena
AU - Lerer, Bernard
AU - Van Broeckhoven, Christine
AU - Mendlewicz, Julien
PY - 2002/3/8
Y1 - 2002/3/8
N2 - Convincing evidence for a genetic component in the etiology of affective disorders (AD), including bipolar affective disorder (BPAD) and unipolar affective disorder (UPAD), is supported by traditional and molecular genetic studies. Most arguments lead to the complex inheritance hypothesis, suggesting that the mode of inheritance is probably not Mendelian but most likely oligogenic (or polygenic) and that the contribution of genes could be moderate or weak. The purpose of the present European multicenter study (13 centers) was to test the potential role in BPAD and UPAD of two candidate dopaminergic markers, DRD2 and DRD3, using a case-control association design. The following samples were analyzed for DRD2: 358 BPAD/358 control (C) and 133 UPAD/133 C subjects, and for DRD3: 325 BPAD/325 C and 136 UPAD/136 C subjects. Patients and controls were individually matched for sex, age (±five years) and geographical origin. Evidence for significant association between BPAD and DRD2 emerged, with an over-representation of genotype 5-5 (P= 0.004) and allele 5 (P=0.002) in BPAD cases compared to controls. No association was found for DRD2 in UPAD, and for DRD3 neither in BPAD or UPAD. Our results suggest that the DRD2 microsatellite may be in linkage disequilibrium with a nearby genetic variant involved in the susceptibility to BPAD. Our large European sample allowed for replicating of some previous reported positive findings obtained in other study populations.
AB - Convincing evidence for a genetic component in the etiology of affective disorders (AD), including bipolar affective disorder (BPAD) and unipolar affective disorder (UPAD), is supported by traditional and molecular genetic studies. Most arguments lead to the complex inheritance hypothesis, suggesting that the mode of inheritance is probably not Mendelian but most likely oligogenic (or polygenic) and that the contribution of genes could be moderate or weak. The purpose of the present European multicenter study (13 centers) was to test the potential role in BPAD and UPAD of two candidate dopaminergic markers, DRD2 and DRD3, using a case-control association design. The following samples were analyzed for DRD2: 358 BPAD/358 control (C) and 133 UPAD/133 C subjects, and for DRD3: 325 BPAD/325 C and 136 UPAD/136 C subjects. Patients and controls were individually matched for sex, age (±five years) and geographical origin. Evidence for significant association between BPAD and DRD2 emerged, with an over-representation of genotype 5-5 (P= 0.004) and allele 5 (P=0.002) in BPAD cases compared to controls. No association was found for DRD2 in UPAD, and for DRD3 neither in BPAD or UPAD. Our results suggest that the DRD2 microsatellite may be in linkage disequilibrium with a nearby genetic variant involved in the susceptibility to BPAD. Our large European sample allowed for replicating of some previous reported positive findings obtained in other study populations.
KW - Affective disorders
KW - Association study
KW - Bipolar affective disorder
KW - Candidate gene
KW - DRD2
KW - DRD3
KW - Dopamine D2 receptor
KW - Dopamine D3 receptor
KW - Unipolar affective disorder
UR - http://www.scopus.com/inward/record.url?scp=18244407076&partnerID=8YFLogxK
UR - https://pubmed.ncbi.nlm.nih.gov/11857579
U2 - 10.1002/ajmg.10118
DO - 10.1002/ajmg.10118
M3 - Article
C2 - 11857579
AN - SCOPUS:18244407076
SN - 1552-4841
VL - 114
SP - 177
EP - 185
JO - American Journal of Medical Genetics, Part B: Neuropsychiatric Genetics
JF - American Journal of Medical Genetics, Part B: Neuropsychiatric Genetics
IS - 2
ER -