A combined analysis of D22S278 marker alleles in affected sib-pairs: Support for a susceptibility locus for schizophrenia at chromosome 22q12

Gill, Michael; Vallada, Homero; Collier, David; Sham, Pak C.; Holmans, Peter; Murray, Robin M.; McGuffin, Peter; Nanko, S.; Owen, Mike; Antonarakis, Stylianos E.; Housman, David E.; Kazazian, Haig H.; Nestadt, Gerald; Pulver, Ann E.; Straub, Richard E.; Maclean, Charles; Walsh, Dermot; Kendler, Kenneth S.; DeLisi, Lynn E.; Polymeropoulos, Mihael H.; Coon, Hilary; Lofthouse, R.; Gershon, Elliot S.; Golden, L.; Crow, Timothy J.; Byerley, William; Freedman, Robert; Laurent, Claudine; Bodeau-Péan, Sylvie; d’Amato, Thierry; Jay, Maurice; Campion, Dominique; Mallet, Jacques; Wildenauer, Dieter B.; Lerer, Bernard; Albus, Margot; Ackenheil, Manfred; Ebstein, Richard P.; Hallmayer, Joachim; Maier, Wolfgang; Gurling, Hugh; Curtis, David; Kalsi, G; Brynjólfsson, Jón; Sigmundson, Thordur; Pétursson, Hannes; Blackwood, Douglas; Muir, Walter; Clair, David St; He, Lin; Maguire, Susan; Moises, Hans W.; Hwu, Hai‐Gwo; Yang, Ling; Wiese, Claudia; Li, Tao; Liu, Xiehe; Kristbjarnason, Helgi; Levinson, Douglas F.; Mowry, Bryan; Donis-Keller, Helen; Hayward, Nicholas K.; Crowe, Raymond R.; Silverman, Jeremy M.; Nancarrow, Derek J.; Read, Christina M.

doi:10.1002/(sici)1096-8628(19960216)67:1<40::aid-ajmg6>3.0.co;2-w

Cited by 215 publications

(83 citation statements)

References 20 publications

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“…12,13,19,20,[60][61][62] They are especially interesting as the same regions may encompass susceptibility genes for schizophrenia. [63][64][65][66][67][68][69][70] Park et al 71 made similar conclusions in a study of psychotic BD in which most areas of linkage overlapped with those reported in previous investigations of schizophrenia.…”

Section: Psychotic Symptoms In Bdsupporting

confidence: 71%

The phenotypes of bipolar disorder: relevance for genetic investigations

2005

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The search for susceptibility genes for bipolar disorder (BD) depends on appropriate definitions of the phenotype. In this paper, we review data on diagnosis and clinical features of BD that could be used in genetic studies to better characterize patients or to define homogeneous subgroups. Clinical symptoms, long-term course, comorbid conditions, and response to prophylactic treatment may define groups associated with more or less specific loci. One such group is characterized by symptoms of psychosis and linkage to 13q and 22q. A second group includes mainly bipolar II patients with comorbid panic disorder, rapid mood switching, and evidence of chromosome 18 linkage. A third group comprises typical BD with an episodic course and favourable response to lithium prophylaxis. Reproducibility of cognitive deficits across studies raises the possibility of using cognitive profiles as endophenotypes of BD, with deficits in verbal explicit memory and executive function commonly reported. Brain imaging provides a more ambiguous data set consistent with heterogeneity of the illness. Keywords: bipolar disorder; genetics; endophenotype; neurocognitive function; brain imaging Bipolar disorder (BD) has a genetic basis with heritability of at least 80%. 1 A number of studies have attempted to map the susceptibility loci giving evidence of linkage in multiple genomic regions. In particular, findings in 4p, 4q, 8q, 10p, 12q24, 13q, 18p, 18q, 21q, and 22q have been supported by more than one study. [2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19] However, these studies have not identified any specific genes, and a recent metaanalysis of available genome scans showed no regions with a conclusive evidence of linkage. 20 The relatively slow progress of gene-mapping efforts is often explained by the 'complex' nature of the illness and of the genotype-phenotype relation. The complexity most likely includes heterogeneity, interactions of multiple loci, incomplete penetrance, as well as phenotypes resulting from environmental effects-either alone or in interaction with the genetic predisposition. The goal of psychiatric genetic research is identification of (heritable) variations in DNA sequence or function that influence behaviour or give rise to mental illness. By definition, in complex (multifactorial) traits, this link is not unique and specific. That is, a particular change in gene sequence does not necessarily lead to a specific behaviour, and similar behaviours (symptoms) may be due to distinct (sets of) genes. Moreover, we must consider the possibility that the path between the genotype and behaviour is not unidirectional. Emerging examples point not only to general effects of environment, for instance stress, on behaviour, but also to specific behaviours influencing gene function that can be transmitted onto the next generation. 21 No single method is considered clearly superior in identifying susceptibility genes for complex traits such as BD. Most researchers agree that a combination of strategies is most lik...

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Section: Psychotic Symptoms In Bdsupporting

confidence: 71%

The phenotypes of bipolar disorder: relevance for genetic investigations

2005

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“…23 The newly discovered synapsin III gene might be a candidate molecule in schizophrenia, 25,26 because of the role of synapsins in neurotransmitter release and synaptogenesis. Reported linkage studies in affected sib pairs showed a hot spot about 4.5 cM from the syn-apsin III gene on chromosome 22, 27 and the region on 22q12 is also associated with the phenotypic measures of inhibitory neurophysiological functioning, P50 auditory sensory gating, and antisaccade ocular motor performance. 28 We tested whether synapsin might also be decreased in the hippocampal formation of schizophrenia using an antibody that measures synapsin Ia, IIa, and IIIa proteins.…”

Section: Introductionmentioning

confidence: 99%

Reduction of synapsin in the hippocampus of patients with bipolar disorder and schizophrenia

et al. 2002

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Several studies suggest that decreased expression of presynaptic proteins may be characteristic of schizophrenia. We examined one such protein, synapsin, in schizophrenia and bipolar disorder. Samples of hippocampal tissue from controls (n = 13), patients with schizophrenia (n = 16), or bipolar disorder (n = 6), and suicide victims (n = 7) were used. The membrane and cytosolic fractions were analyzed by Western immunoblotting for synapsin using an antibody that detects synapsin Ia, IIa, and IIIa proteins. Synaptophysin was also measured for comparison. Total synapsin was decreased significantly in patients with schizophrenia (P = 0.034) and in bipolar disorder (P = 0.00008) as compared to controls. The synapsin/synaptophysin ratios were decreased in schizophrenia and bipolar disorder, and additionally in suicide victims (P = 0.014). Age, postmortem interval, percentage of protein extracted, and pH of brain were not different between groups. No changes in total synapsin or synaptophysin in the hippocampus were produced by injecting rats with either lithium or haloperidol for 30 days. Reductions in synapsin in both patients with schizophrenia (synapsin IIa and IIIa) and bipolar disorder (synapsin Ia, IIa and IIIa) imply that altered or reduced synaptic function in the hippocampus may be involved in these disorders.

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“…In parallel to these two major developments, incremental but important progress has been made due to the coordination of genome-wide scans with more targeted replication studies of promising regions by worldwide consortia. [12][13][14][15] Many regions now have support from multiple independent studies, although due to major methodological differences between studies, the cumulative strength of the evidence for each locus remains difficult to judge. Recent reviews, [16][17][18][19][20] when taken together, provide a fairly comprehensive catalog of the most positive studies, but it is likely that negative results are substantially under-represented in the literature.…”

Section: Introductionmentioning

confidence: 99%

Genome-wide scans of three independent sets of 90 Irish multiplex schizophrenia families and follow-up of selected regions in all families provides evidence for multiple susceptibility genes

et al. 2002

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From our linkage study of Irish families with a high density of schizophrenia, we have previously reported evidence for susceptibility genes in regions 5q21-31, 6p24-21, 8p22-21, and 10p15-p11. In this report, we describe the cumulative results from independent genome scans of three a priori random subsets of 90 families each, and from multipoint analysis of all 270 families in ten regions. Of these ten regions, three (13q32, 18p11-q11, and 18q22-23) did not generate scores above the empirical baseline pairwise scan results, and one (6q13-26) generated a weak signal. Six other regions produced more positive pairwise and multipoint results. They showed the following maximum multipoint H-LOD (heterogeneity LOD) and NPL scores: 2p14-13: 0.89 (P = 0.06) and 2.08 (P = 0.02), 4q24-32: 1.84 (P = 0.007) and 1.67 (P = 0.03), 5q21-31: 2.88 (P = 0.0007), and 2.65 (P = 0.002), 6p25-24: 2.13 (P = 0.005) and 3.59 (P = 0.0005), 6p23: 2.42 (P = 0.001) and 3.07 (P = 0.001), 8p22-21: 1.57 (P = 0.01) and 2.56 (P = 0.005), 10p15-11: 2.04 (P = 0.005) and 1.78 (P = 0.03). The degree of 'internal replication' across subsets differed, with 5q, 6p, and 8p being most consistent and 2p and 10p being least consistent. On 6p, the data suggested the presence of two susceptibility genes, in 6p25-24 and 6p23-22. Very few families were positive on more than one region, and little correlation between regions was evident, suggesting substantial locus heterogeneity. The levels of statistical significance were modest, as expected from loci contributing to complex traits. However, our internal replications, when considered along with the positive results obtained in multiple other samples, suggests that most of these six regions are likely to contain genes that influence liability to schizophrenia.

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A combined analysis of D22S278 marker alleles in affected sib-pairs: Support for a susceptibility locus for schizophrenia at chromosome 22q12

Cited by 215 publications

References 20 publications

The phenotypes of bipolar disorder: relevance for genetic investigations

The phenotypes of bipolar disorder: relevance for genetic investigations

Reduction of synapsin in the hippocampus of patients with bipolar disorder and schizophrenia

Genome-wide scans of three independent sets of 90 Irish multiplex schizophrenia families and follow-up of selected regions in all families provides evidence for multiple susceptibility genes

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