A Prospective Cohort Study of Genetic and Perinatal Influences in the Etiology of Schizophrenia

Td, Cannon; Rosso, Isabelle M.; Jm, Hollister; Bearden, Carrie E.; Le, Sanchez; Hadley, Trevor R.

doi:10.1093/oxfordjournals.schbul.a033458

Cited by 193 publications

(162 citation statements)

References 88 publications

(127 reference statements)

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“…1,5,[7][8][9][10] A recent review by Schmidt-Kastner and colleagues 11 suggested that susceptibility genes for schizophrenia were more likely than randomly selected genes to be regulated by hypoxia/ischemia and/or expressed in the cerebrovasculature. In fact, a substantial fraction of the genes reported to be significantly associated with schizophrenia in at least two published studies fit this description, even though only 1-2% of known genes are involved in hypoxia-induced regulation.…”

Section: Introductionmentioning

confidence: 99%

Serious obstetric complications interact with hypoxia-regulated/vascular-expression genes to influence schizophrenia risk

et al. 2008

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The etiology of schizophrenia is thought to include both epistasis and gene-environment interactions. We sought to test whether a set of schizophrenia candidate genes regulated by hypoxia or involved in vascular function in the brain (AKT1, BDNF, CAPON, CHRNA7, COMT, DTNBP1, GAD1, GRM3, NOTCH4, NRG1, PRODH, RGS4, TNF-a) interacted with serious obstetric complications to influence risk for schizophrenia. A family-based study of transmission disequilibrium was conducted in 116 trios. Twenty-nine probands had at least one serious obstetric complication (OC) using the McNeil-Sjostrom Scale, and many of the OCs reported were associated with the potential for fetal hypoxia. Analyses were conducted using conditional logistic regression and a likelihood ratio test (LRT) between nested models was performed to assess significance. Of the 13 genes examined, four (AKT1 (three SNPs), BDNF (two SNPs), DTNBP1 (one SNP) and GRM3 (one SNP)) showed significant evidence for gene-by-environment interaction (LRT P-values ranged from 0.011 to 0.037). Although our sample size was modest and the power to detect interactions was limited, we report significant evidence for genes involved in neurovascular function or regulated by hypoxia interacting with the presence of serious obstetric complications to increase risk for schizophrenia.

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Section: Introductionmentioning

confidence: 99%

Serious obstetric complications interact with hypoxia-regulated/vascular-expression genes to influence schizophrenia risk

et al. 2008

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“…The heritability of performance deficits on measures of executive function, vigilance, and declarative memory has been demonstrated in twin studies (Cannon et al, 2000;Goldberg et al, 1990) and in studies of first degree relatives Faraone et al, 1995). This has lead to the suggestion that genetic liability for schizophrenia is at least partly mediated by deleterious effects on the brain regions associated with these cognitive functions, including pre-frontal and medial temporal lobe regions (Weinberger et al, 2001 Recent reviews of schizophrenia genetics (Craddock, O'Donovan, & Owen, 2005) have highlighted the potential role of a number of candidate genes in conferring liability to the disorder.…”

Section: Introductionmentioning

confidence: 99%

Variance in neurocognitive performance is associated with dysbindin-1 in schizophrenia: A preliminary study

et al. 2007

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Susceptibility genes for schizophrenia have been hypothesised to mediate liability for the disorder at least partly by influencing cognitive performance. We investigated the association between genotype and cognitive performance for a Dysbindin risk haplotype which is associated with schizophrenia in our sample. Fifty-two patients with schizophrenia or schizoaffective disorder (24 risk haplotypes carriers versus 28 non-risk haplotype carriers) were assessed in areas of cognition showing evidence of familial deficits in schizophrenia. Verbal and spatial memory, working memory, and attentional control was assessed using selected measures from the Weschler memory scale (WMS), Cambridge automated test battery (CANTAB), continuous performance test (CPT), and a simple go/no-go task. Pre-morbid IQ was also assessed using the Weschler Test of Adult Reading (WTAR). Patients carrying the Dysbindin risk haplotype showed significantly lower spatial working memory performance than patients who were non-risk carriers, with genotype explaining 12% of variance in performance. Our study suggests that the increased risk for schizophrenia associated with dysbindin may be partly mediated by its influence on pre-frontal function.

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“…For example, DHEA and DHEAS decrease neuronal death following anoxia (Marx et al, 2000b), and obstetrical complications resulting in hypoxia are associated with increased schizophrenia risk (Dalman et al, 2001;Cannon et al, 1999Cannon et al, , 2000Geddes et al, 1999). Allopregnanolone demonstrates anticonvulsant actions in a number of seizure paradigms (Kokate et al, 1994(Kokate et al, , 1996Devaud et al, 1995;Belelli et al, 1989) and exhibits pronounced protective effects against neurodegeneration in a mouse model of Niemann-Pick type C disease .…”

Section: Introductionmentioning

confidence: 99%

Neuroactive Steroids are Altered in Schizophrenia and Bipolar Disorder: Relevance to Pathophysiology and Therapeutics

Marx

Stevens

Shampine

et al. 2005

Neuropsychopharmacol

155

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Evidence suggests that neuroactive steroids may be candidate modulators of schizophrenia pathophysiology and therapeutics. We therefore investigated neuroactive steroid levels in post-mortem brain tissue from subjects with schizophrenia, bipolar disorder, nonpsychotic depression, and control subjects to determine if neuroactive steroids are altered in these disorders. Posterior cingulate and parietal cortex tissue from the Stanley Foundation Neuropathology Consortium collection was analyzed for neuroactive steroids by negative ion chemical ionization gas chromatography/mass spectrometry preceded by high-performance liquid chromatography. Subjects with schizophrenia, bipolar disorder, nonpsychotic depression, and control subjects were group matched for age, sex, ethnicity, brain pH, and post-mortem interval (n ¼ 14-15 per group, 59-60 subjects total). Statistical analyses were performed by ANOVA with post-hoc Dunnett tests on log transformed neuroactive steroid levels. Pregnenolone and allopregnanolone were present in human post-mortem brain tissue at considerably higher concentrations than typically observed in serum or plasma. Pregnenolone and dehydroepiandrosterone levels were higher in subjects with schizophrenia and bipolar disorder compared to control subjects in both posterior cingulate and parietal cortex. Allopregnanolone levels tended to be decreased in parietal cortex in subjects with schizophrenia compared to control subjects. Neuroactive steroids are present in human post-mortem brain tissue at physiologically relevant concentrations and altered in subjects with schizophrenia and bipolar disorder. A number of neuroactive steroids act at inhibitory GABA A and excitatory NMDA receptors and demonstrate neuroprotective and neurotrophic effects. Neuroactive steroids may therefore be candidate modulators of the pathophysiology of schizophrenia and bipolar disorder, and relevant to the treatment of these disorders.

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A Prospective Cohort Study of Genetic and Perinatal Influences in the Etiology of Schizophrenia

Cited by 193 publications

References 88 publications

Serious obstetric complications interact with hypoxia-regulated/vascular-expression genes to influence schizophrenia risk

Serious obstetric complications interact with hypoxia-regulated/vascular-expression genes to influence schizophrenia risk

Variance in neurocognitive performance is associated with dysbindin-1 in schizophrenia: A preliminary study

Neuroactive Steroids are Altered in Schizophrenia and Bipolar Disorder: Relevance to Pathophysiology and Therapeutics

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