TY - JOUR
T1 - Possible linkage of schizophrenia and bipolar affective disorder to chromosome 3q29: A follow-up
AU - Schosser, Alexandra
AU - Fuchs, Karoline
AU - Leisch, Friedrich
AU - Bailer, Ursula
AU - Meszaros, Kurt
AU - Lenzinger, Elisabeth
AU - Willinger, Ulrike
AU - Strobl, Rainer
AU - Heiden, Angela
AU - Gebhardt, Christian
AU - Kasper, Siegfried
AU - Sieghart, Werner
AU - Hornik, Kurt
AU - Aschauer, Harald
N1 - Coden: JPYRA
Affiliations: Department of General Psychiatry, University Hospital for Psychiatry, A-1090 Vienna, Austria; Brain Research Institute, University of Vienna, Div. of Biochem. and Molec. Biology, A-1090 Vienna, Austria; Institut fu?r Statistik, Decision Support Systems, University Wien, A-1010 Vienna, Austria; Dept. Social Psychiat. Eval. Res., University Hospital for Psychiatry, A-1090 Vienna, Austria; Inst. F. Stat. W., University of Technology, A-1040 Vienna, Austria
Adressen: Schosser, A.; Department of General Psychiatry; University Hospital for Psychiatry A-1090 Vienna, Austria; email: [email protected]
Source-File: Psy472Scopus.csv
Import aus Scopus: 2-s2.0-10744220779
Importdatum: 08.01.2007 17:33:29
15.01.2009: Datenanforderung 2652 (Import Sachbearbeiter)
09.02.2010: Datenanforderung UNIVIS-DATEN-DAT.RA-2 (Import Sachbearbeiter)
PY - 2004
Y1 - 2004
N2 - The present linkage study is a follow-up within the chromosome 3q29 region in schizophrenia and bipolar affective disorder families, based on our recently published genome scan, resulting in evidence for linkage of both disorders to this region (marker D3S1265: NPL [non parametric lod] score Z all=3.74, P=0.003). Using the same family sample (five pedigrees with schizophrenic index patients and three pedigrees with index bipolar disorder patients N†; 50 of them were available for genotyping), genotyping of eight additional markers close to D3S1265 was done. Five of those new markers (three centromeric and two telomeric of D3S1265) spanning 4.14 cM (centiMorgan) could be used for statistical analyses ("new markers"). Moreover, marker D3S1265, genotyped within the published genome scan, was used for additional calculations. Linkage analysis was performed using the GENEHUNTER program version 2.1r3. Within newly genotyped markers the highest NPL score Zall observed was 1.93296 with the telomeric SNP (single nucleotide polymorphism) rs1835669, corresponding to P=0.032166. Statistical analysis including D3S1265, located in between the newly genotyped markers, resulted in a peak NPL score Zall=4.00179 with marker D3S1265, that is P=0.000128. Doing subset analyses of the bipolar disorder and schizophrenia families separately with new markers and D3S1265, linkage signals arose substantially from bipolar disorder families, with contribution from schizophrenia families, too. The results of our follow-up study support our previous linkage finding of schizophrenia and bipolar affective disorder to chromosome 3q29. Œ 2003 Elsevier Ltd. All rights reserved.
AB - The present linkage study is a follow-up within the chromosome 3q29 region in schizophrenia and bipolar affective disorder families, based on our recently published genome scan, resulting in evidence for linkage of both disorders to this region (marker D3S1265: NPL [non parametric lod] score Z all=3.74, P=0.003). Using the same family sample (five pedigrees with schizophrenic index patients and three pedigrees with index bipolar disorder patients N†; 50 of them were available for genotyping), genotyping of eight additional markers close to D3S1265 was done. Five of those new markers (three centromeric and two telomeric of D3S1265) spanning 4.14 cM (centiMorgan) could be used for statistical analyses ("new markers"). Moreover, marker D3S1265, genotyped within the published genome scan, was used for additional calculations. Linkage analysis was performed using the GENEHUNTER program version 2.1r3. Within newly genotyped markers the highest NPL score Zall observed was 1.93296 with the telomeric SNP (single nucleotide polymorphism) rs1835669, corresponding to P=0.032166. Statistical analysis including D3S1265, located in between the newly genotyped markers, resulted in a peak NPL score Zall=4.00179 with marker D3S1265, that is P=0.000128. Doing subset analyses of the bipolar disorder and schizophrenia families separately with new markers and D3S1265, linkage signals arose substantially from bipolar disorder families, with contribution from schizophrenia families, too. The results of our follow-up study support our previous linkage finding of schizophrenia and bipolar affective disorder to chromosome 3q29. Œ 2003 Elsevier Ltd. All rights reserved.
U2 - 10.1016/j.jpsychires.2003.11.004
DO - 10.1016/j.jpsychires.2003.11.004
M3 - Article
VL - 38
SP - 357
EP - 364
JO - Journal of Psychiatric Research
JF - Journal of Psychiatric Research
SN - 0022-3956
IS - 3
ER -