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Query: UMLS:C0036341 (
schizophrenia
)
60,220
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The hypothesis that pathologic immune mechanisms, characterized by production of brain autoantibodies, operate in
schizophrenia
, was the basis for this study. Binding of serum globulin substance by human brain septal region obtained at autopsy was measured by radioimmunofixation assay in 27 schizophrenic probands, 28 first-degree relatives, 12 patients with primary affective disorder (depression), and 117 normal controls. Schizophrenic individuals tended to have higher levels of brain-serum affinity than controls. Age and sex did not appear to affect results. Within families, elevation of serum-binding activity showed intra sib-pair resemblance, distinguished healthy relatives from probands and ill relatives and relatives of probands with positive sera from relatives of probands with negative serum activity. Serum activity distinguished well relatives from normal controls and was independent of clinical state. This suggests that brain-serum affinity may be compatible with characteristics of a genetic marker of vulnerability to
schizophrenia
. Within sib-pairs, concordance rates for elevated serum activity and for subtype diagnosis, mode, and age of illness onset were positively related. This finding supports clinico-genetic disposition in a subgroup of schizophrenic persons. To determine distribution patterns of antigenic components, selected schizophrenic and normal sera were tested against human liver and mouse brain,
thymus
, and liver. Wide tissue cross-reactivity was observed in schizophrenic, but not in normal sera, a finding consistent with overlap of serological reactions affecting specific tissues in autoimmune processes. The assay employed in the present study and investigation of inheritance of brain-serum affinity have not previously been reported.
...
PMID:Tissue-binding factor in schizophrenic sera: a clinical and genetic study. 87 93
Sera from healthy people and from patients with
schizophrenia
were heated at 56 degrees for 30 min and then kept at 4 degrees . These sera were then tested for cytotoxicity and by the indirect immunofluorescence method with thymocytes, bone-marrow cells, and lymph-node cells of adult C(3)H mice. The cytotoxicity index for mouse thymocytes of sera from 60 healthy donors ranged from 0.00 to 0.4, with an average of 0.08. That of sera from 35 patients with
schizophrenia
ranged from 0.29 to 0.91, with an average of 0.71. The cytotoxicity index for mouse bone-marrow cells of sera from healthy donors ranged from 0.03 to 0.23, whereas that of sera from patients with
schizophrenia
ranged from 0.00 to 0.14. Sera of patients at dilutions of 1:8-1:32 displayed immunofluorescence of almost 100% of thymocytes and 58-78% of lymphocytes, whereas sera of healthy donors displayed none. We thus conclude that the sera of patients with
schizophrenia
contain antibodies against thymic antigens localized on thymocytes and
thymus
-derived lymphocytes.
...
PMID:Antibodies to thymocytes in sera of patients with schizophrenia. 458 94
To investigate molecular and clinical aspects of conotruncal anomaly face (CAF), we studied the correlation between deletion size and phenotype and the mode of inheritance in 183 conotruncal anomaly face syndrome (CAFS) patients. Hemizygosity for a region of 22ql1.2 was found in 180 (98%) of the patients with CAFS by fluorescence in situ hybridization (FISH) using the N25(D22S75) DiGeorge critical region (DGCR) probe. No hemizygosity was found in three (2%) of the patients with CAFS by FISH using nine DiGeorge critical region probes and a SD1OP1 probe (DGA II locus). None of these three patients had mental retardation and just one had nasal intonation, which was observed in almost all of the 180 CAFS patients who carried deletions (mental retardation, 92%; nasal voice, 88%). Nineteen of 143 families (13%) had familial CAFS and 16 affected parents (84%) were mothers. Although only two of the affected parents had cardiovascular anomalies, the deletion size in the 16 affected parents and their affected family members, who were studied by FISH analysis, was the same. It indicates that extragenic factors may play a role in the genesis of phenotypic variability, especially in patients with cardiovascular anomalies. No familial cases were found among CAFS patients with absent
thymus
/DiGeorge anomaly (DGA). Also, in all 18 CAFS patients with completely absent
thymus
/DGA and all 6 CAFS patients with
schizophrenia
, it was revealed that the deletion was longer distally. A study of the origin of the deletion using microsatellite analyses in 48 de novo patients showed that in 65% of CAFS patients it was maternal, while in 64% of DGA patients it was paternal. The findings of this study indicated that CAF was almost always associated with the deletion of 22ql1.2. As well as the major features of the syndrome, other notable extracardiac anomalies were found to be susceptibility to infection,
schizophrenia
, atrophy or dysmorphism of the brain, thrombocytopenia, short stature, facial palsy, anal atresia, and mild limb abnormalities.
...
PMID:Molecular and clinical study of 183 patients with conotruncal anomaly face syndrome. 973 80
22q11 deletion syndrome (22q11DS) is a chromosomal disorder that results in variable multisystem abnormalities, including conotruncal cardiac malformations, aplasia or hypoplasia of the
thymus
and/or parathyroid glands, immunodeficiency, dysmorphic facial features, and cleft palate and other nasopharyngeal and dental anomalies. Individuals with 22q11DS also exhibit cognitive and behavioral difficulties, including delayed motor and speech-language development, mental retardation, low academic achievement, impaired spatial reasoning, poor attentional and executive functioning, attention-deficit hyperactivity disorder, autism spectrum disorders, mood disorders, and/or
schizophrenia
spectrum disorders. Interventions should be designed based on the results of periodic developmental and neuropsychological assessments and psychiatric screening. Future research should focus on understanding deletion-related gene-environment interactions and their effects on developmental and behavioral outcomes, identifying neurodegenerative processes in 22q11DS, and developing preventive models of behavioral and psychopharmacologic treatment.
...
PMID:A review of neurocognitive and behavioral profiles associated with 22q11 deletion syndrome: implications for clinical evaluation and treatment. 1738 27
We propose a unifying hypothesis of
schizophrenia
to help reconcile findings from many different disciplines. This hypothesis proposes that
schizophrenia
often involves pre- or perinatal exposure to adverse factors that produce a latent immune vulnerability. When this vulnerability is manifested, beginning around puberty with changes in immune function and involution of the
thymus
, individuals become more susceptible to infections and immune dysfunctions that contribute to
schizophrenia
. Our hypothesis suggests theoretical bridges between different lines of evidence on
schizophrenia
and offers explanations for many puzzling findings about
schizophrenia
. For example, the hypothesis helps account for why
schizophrenia
patients tend to have had increased exposure to neurotropic infections, but most individuals with such exposure do not develop
schizophrenia
, and why prenatal hardships increase risk for
schizophrenia
, but the onset of symptoms typically does not occur until after puberty. The hypothesis also explains another paradox: lower socioeconomic status and poor prenatal care increase risk for
schizophrenia
at the same geographic site, but international comparisons indicate that countries with higher per capita incomes and better prenatal care actually tend to have higher
schizophrenia
prevalences. As the hypothesis predicts, (1) prenatal adversity, which increases risk for
schizophrenia
, also impairs post-pubertal immune competence, (2)
schizophrenia
patients experience elevated morbidity from infectious and auto-immune diseases, (3) genetic and environmental risk factors for
schizophrenia
increase vulnerability to these diseases, (4) factors that exacerbate schizophrenic symptoms also tend to impair immune function, (5) many anti-psychotic medications combat infection, (6) effects of early infections may not appear until after puberty, when they can produce neurologic and psychiatric symptoms, and (7) immune dysfunctions, such as imbalances of pro- and anti-inflammatory cytokines, may contribute to the onset of psychotic symptoms and the progressive loss of brain tissue in
schizophrenia
. The disruptive effects of prenatal adversity on the development of the immune system may often combine with adverse effects on prenatal brain development to produce
schizophrenia
. This paper focuses on the adverse immune system effects, because effects on the brain have been extensively discussed in neurodevelopmental theories of
schizophrenia
. We propose new tests of scientific predictions. We also point out potential clinical implications of the hypothesis; for example, individuals with
schizophrenia
may often have underlying infections or immune dysfunctions, such as imbalances in inflammatory cytokines, that contribute to the illness. This possibility could be tested experimentally--e.g., by clinical trials in which patients' exposure to infection is reduced or immune function is normalized.
...
PMID:A unifying hypothesis of schizophrenia: abnormal immune system development may help explain roles of prenatal hazards, post-pubertal onset, stress, genes, climate, infections, and brain dysfunction. 1983 3
ZNF804a was identified by a genome-wide association study (GWAS) in which a single nucleotide polymorphism (SNP rs1344706) in ZNF804a reached genome-wide statistical significance for association with a combined diagnosis of
schizophrenia
(SZ) and bipolar disorder. Although the molecular function of ZNF804a is unknown, the amino acid sequence is predicted to contain a C2H2-type zinc-finger domain and suggests ZNF804a plays a role in DNA binding and transcription. Here, we confirm that ZNF804a directly contributes to transcriptional control by regulating the expression of several SZ associated genes and directly interacts with chromatin proximal to the promoter regions of
PRSS16
and COMT, the two genes we find upregulated by ZNF804a. Using immunochemistry we establish that ZNF804a is localized to the nucleus of rat neural progenitor cells in culture and in vivo. We demonstrate that expression of ZNF804a results in a significant increase in transcript levels of
PRSS16
and COMT, relative to GFP transfected controls, and a statistically significant decrease in transcript levels of PDE4B and DRD2. Furthermore, we show using chromatin immunoprecipitation assays (ChIP) that both epitope-tagged and endogenous ZNF804a directly interacts with the promoter regions of
PRSS16
and COMT, suggesting a direct upregulation of transcription by ZNF804a on the expression of these genes. These results are the first to confirm that ZNF804a regulates transcription levels of four SZ associated genes, and binds to chromatin proximal to promoters of two SZ genes. These results suggest a model where ZNF804a may modulate a transcriptional network of SZ associated genes.
...
PMID:ZNF804a regulates expression of the schizophrenia-associated genes PRSS16, COMT, PDE4B, and DRD2. 2238 43
Recent GWAS demonstrated an association between candidate genes located at region 6p22.1 and
schizophrenia
. This region has been reported to house certain candidate SNPs, which may be associated with
schizophrenia
at HIST1H2BJ,
PRSS16
, and PGBD1. These genes may presumably be associated with pathophysiology in
schizophrenia
, namely epigenetics and psychoneuroimmunology. A three-step study was undertaken to focus on these genes with the following aims: (1) whether these genes may be associated in Japanese patients with
schizophrenia
by performing a 1st stage case-control study (514 cases and 706 controls) using Japanese tagging SNPs; (2) if the genetic regions of interest for the disease from the 1st stage of analyses were found, re-sequencing was performed to search for new mutations; (3) finally, a replication study was undertaken to confirm positive findings from the 1st stage were reconfirmed using a larger number of subjects (2,583 cases and 2,903 controls) during a 2nd stage multicenter replication study in Japan. Genotyping was performed using TaqMan PCR method for the selected nine tagging SNPs. Although three SNPs situated at the 3' side of PGBD1; rs3800324, rs3800327, and rs2142730, and two-window haplotypes between rs3800327 and rs2142730 showed positive associations with
schizophrenia
, these associations did not have enough power to sustain significance during the 2nd stage replication study. In addition, re-sequencing for exons 5 and 6 situated at this region did not express any new mutations for
schizophrenia
. Taken together these results indicate that the genes HIST1H2BJ,
PRSS16
, and PGBD1 were not associated with Japanese patients with
schizophrenia
.
...
PMID:No associations found between the genes situated at 6p22.1, HIST1H2BJ, PRSS16, and PGBD1 in Japanese patients diagnosed with schizophrenia. 2248 95
Chronic psychosocial stress is a recognized risk factor for various affective and somatic disorders. In an established murine model of chronic psychosocial stress, exposure to chronic subordinate colony housing (CSC) results in an alteration of physiological, behavioral, neuroendocrine and immunological parameters, including a long-lasting increase in anxiety, adrenal hypertrophy and
thymus
atrophy. Based on the stress-protective and anxiolytic properties of oxytocin (OXT) after acute administration in rodents and humans, the major aims of our study were to assess whether chronic administration of OXT dose-dependently affects the behavior and physiology of male mice, as for therapeutic use in humans, mostly chronic treatment approaches will be used. Further, we studied, whether chronic administration during CSC prevents stress-induced consequences. Our results indicate that chronic intracerebroventricular (ICV) infusion of OXT (15 days) at high (10ng/h), but not at low (1ng/h) dose, induces an anxiogenic phenotype with a concomitant reduction of OXT receptor (OXTR) binding within the septum, the basolateral and medial amygdala, as well as the median raphe nucleus. Further, we demonstrate that chronic ICV infusion of OXT (1ng/h) during a 19-day CSC exposure prevents the hyper-anxiety,
thymus
atrophy, adrenal hypertrophy, and decreased in vitro adrenal ACTH sensitivity. Thus, given both negative, but also beneficial effects seen after chronic OXT treatment, which appear to be dose-dependent, a deeper understanding of long-lasting treatment effects is required before OXT can be considered for long-term therapeutic use for the treatment of psychopathologies such as autism,
schizophrenia
or anxiety-disorders.
...
PMID:Dose-dependent effects of chronic central infusion of oxytocin on anxiety, oxytocin receptor binding and stress-related parameters in mice. 2463 19
Extensive research implicates disturbed immune function and development in the etiology and pathology of
schizophrenia
. In addition to reviewing evidence for immunological factors in
schizophrenia
, this paper discusses how an emerging model of atypical immune function and development helps explain a wide variety of well-established - but puzzling - findings about
schizophrenia
. A number of theorists have presented hypotheses that early immune system programming, disrupted by pre- and perinatal adversity, often combines with abnormal brain development to produce
schizophrenia
. The present paper focuses on the hypothesis that disruption of early immune system development produces a latent immune vulnerability that manifests more fully after puberty, when changes in immune function and the
thymus
leave individuals more susceptible to infections and immune dysfunctions that contribute to
schizophrenia
. Complementing neurodevelopmental models, this hypothesis integrates findings on many contributing factors to
schizophrenia
, including prenatal adversity, genes, climate, migration, infections, and stress, among others. It helps explain, for example, why (a)
schizophrenia
onset is typically delayed until years after prenatal adversity, (b) individual risk factors alone often do not lead to
schizophrenia
, and (c)
schizophrenia
prevalence rates actually tend to be higher in economically advantaged countries. Here we discuss how the hypothesis explains 10 key findings, and suggests new, potentially highly cost-effective, strategies for treatment and prevention of
schizophrenia
. Moreover, while most human research linking immune factors to
schizophrenia
has been correlational, these strategies provide ethical ways to experimentally test in humans theories about immune function and
schizophrenia
. This article is part of a Special Issue entitled SI: Neuroimmunology in Health And Disease.
...
PMID:Abnormal immune system development and function in schizophrenia helps reconcile diverse findings and suggests new treatment and prevention strategies. 2573 81
Schizophrenia
is a severe debilitating psychiatric disorder, with a typical onset in adolescence or early adulthood. This condition is characterized by heterogeneous symptoms (hallucinations, delusions, disorganized behaviour, affective flattening, and social isolation) and a life-time prevalence of 0.5-1.2%. In spite of the efforts to uncover the etiology of the disorder, its pathogenesis and neurobiological background are poorly understood. Given the high heritability in
schizophrenia
, genetic research remains an important area of focus. Besides the common variations of low penetrance - single nucleotid polymorphisms (SNPs) -, rare variants, mainly copy number variations (CNVs) play a role in the genetic architecture of the disorder. The most frequent CNV associated with
schizophrenia
is the hemizygous deletion of the 22q11.2 region. According to previous research this genetic variant occurs in 1% of the patients and conversely, 25% of the carriers of the 22q11.2 microdeletion will develop
schizophrenia
. The 22q11.2 deletion syndrome (22Q11DS, velocardiofacial (VCFS) syndrome, DiGeorge-syndrome) is usually a childhood diagnosis. Its prevalence is 1:2000-4000 considering all births. Patients can demonstrate heart developmental disorders, craniofacial (elongated face, hypertelorism), immunological (
thymus
-hypoplasia), endocrinological (hypocalcaemia) abnormalities, and neurodevelopmental alterations, but only a proportion will have these abnormalities due to incomplete penetrance. The variable symptoms complicate the recognition of the syndrome in the day to day medical practice. 25% of the known 22Q11DS patients develop
schizophrenia
but the risk of neuropsychiatric problems, like autism, ADHD and childhood conduct disorder is also increased, while early onset Parkinson's disease in also more frequent in adults. The
schizophrenia
phenotype is not distinguishable at the moment in patients with or without the 22q11 deletion. But emerging evidence suggests that early onset Parkinson's disease is more frequent in 22Q11DS and the effects of clozapine treatment could be different in
schizophrenia
with 22Q11DS. The question arises what is the incidence rate of the 22q11.2 microdeletion among our Hungarian DNA samples with
schizophrenia
. To answer the question, we utilized a new method used in routine genetic diagnostics, multiplex ligation-based probe amplification (MLPA). Although we genotyped the DNA of 315 Hungarian
schizophrenia
patients, we found no 22Q11DS in this cohort. The findings are discussed in terms of basic research and their translation into everyday clinical practice.
...
PMID:[An attempt to identify 22q11.2 microdeletions in samples of the Hungarian schizophrenia DNA bank by multiplex ligation-based probe amplification (MLPA): literature review, methodology and results]. 2825 64
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