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Drug
Enzyme
Compound
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Query: UMLS:C0036341 (
schizophrenia
)
60,220
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Recent studies have suggested that RTN4 is a multifunctional gene, including inhibition of axonal regeneration, vascular remodeling, apoptosis, and tumor suppression. The TATC and
CAA
insertion/deletion polymorphisms of RTN4 3'-UTR have been linked to
schizophrenia
, depression, and dilated cardiomyopathy. To test whether these two polymorphisms are associated with cervical squamous cell carcinoma (CSCC), in this research, by using polymerase chain reaction-polyacrylamide gel electrophoresis, we determined the genotypes of the TATC and
CAA
polymorphisms in 336 CSCC patients and 450 unrelated control subjects. Allele frequencies of TATC and
CAA
polymorphisms were not significantly different between CSCC patients and control subjects (odds ratio [OR]=1.22, 95% confidence interval [CI]=0.98-1.50 for TATC; OR=0.95, 95% CI=0.76-1.18 for
CAA
). Decreased CSCC risk was associated with TATC polymorphism in a recessive model (OR=0.49, 95% CI=0.30-0.77), while no significant association was observed between
CAA
polymorphism and CSCC in different genetic models. Results of stratified analysis revealed that both TATC and
CAA
polymorphisms were associated with high clinical stage, and
CAA
polymorphism was also associated with positive parametrial invasion (OR=0.69, 95% CI=0.48-0.98). The present study provides evidence that TATC and
CAA
insertion/deletion polymorphisms are associated with CSCC, indicating that genetic variation in RTN4 3'-UTR contributes to the susceptibility to CSCC. It is necessary to confirm these findings in ethnically different populations and with a larger sample.
...
PMID:Genetic variation in RTN4 3'-UTR and susceptibility to cervical squamous cell carcinoma. 2232 Aug 44
The aetiology of
schizophrenia
is still unknown but it involves both heritable and non-heritable factors. DNA methylation is an inheritable epigenetic modification that stably alters gene expression. It takes part in the regulation of neurodevelopment and may be a contributing factor to the pathogenesis of brain diseases. It was found that many of the antipsychotic drugs may lead to epigenetic modifications. We have performed 42 high-resolution genome-wide methylation array analyses to determine the methylation status of 27,627 CpG islands. Differentially methylated regions were studied with samples from 20 Bulgarian individuals divided in four groups according to their gender (12 males/8 females) and their treatment response (6 in complete/14 in incomplete remission). They were compared to two age and sex matched control pools (110 females in female pool/110 males in male pool) before and after treatment. We found significant differences in the methylation profiles between male
schizophrenia
patients with complete remission and control male pool before treatment (
C16orf70
,
CST3
,
DDRGK1
,
FA2H
,
FLJ30058
,
MFSD2B
,
RFX4
,
UBE2J1
,
ZNF311
) and male
schizophrenia
patients with complete remission and control male pool after treatment (
AP1S3
,
C16orf59
,
KCNK15
,
LOC146336
,
MGC16384
,
XRN2
) that potentially could be used as target genes for new therapeutic strategies as well as markers for good treatment response. Our data revealed major differences in methylation profiles between male
schizophrenia
patients in complete remission before and after treatment and healthy controls which supports the hypothesis that antipsychotic drugs may play a role in epigenetic modifications.
...
PMID:Whole genome methylation analyses of schizophrenia patients before and after treatment. 2601 38
Genome-wide association studies (GWAS) and proteomic studies have provided convincing evidence implicating alterations in immune/inflammatory processes in
schizophrenia
. However, despite the convergence of evidence, direct links between the genetic and proteomic findings are still lacking for
schizophrenia
. We investigated associations between single nucleotide polymorphisms (SNPs) from the custom-made PsychArray and the expression levels of 190 multiplex immunoassay profiled serum proteins in 149
schizophrenia
patients and 198 matched controls. We identified associations between 81 SNPs and 29 proteins, primarily involved in immune/inflammation responses. Significant SNPxDiagnosis interactions were identified for eight serum proteins including Factor-VII[rs555212], Alpha-1-Antitrypsin[rs11846959], Interferon-Gamma Induced Protein 10[rs4256246] and von-Willebrand-Factor[rs12829220] in the control group; Chromogranin-A[rs9658644],
Cystatin-C
[rs2424577] and Vitamin K-Dependent Protein S[rs6123] in the
schizophrenia
group; Interleukin-6 receptor[rs7553796] in both the control and
schizophrenia
groups. These results suggested that the effect of these SNPs on expression of the respective proteins varies with diagnosis. The combination of patient-specific genetic information with blood biomarker data opens a novel approach to investigate disease mechanisms in
schizophrenia
and other psychiatric disorders. Our findings not only suggest that blood protein expression is influenced by polymorphisms in the corresponding gene, but also that the effect of certain SNPs on expression of proteins can vary with diagnosis.
...
PMID:Associations between SNPs and immune-related circulating proteins in schizophrenia. 2897 76
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