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Association between the MnSOD Ala-9Val polymorphism and development of schizophrenia and abnormal involuntary movements in the Xhosa population
Authors:Hitzeroth Angelika  Niehaus Dana J H  Koen Liezl  Botes Willem C  Deleuze J F  Warnich Louise
Institution:Department of Genetics, Stellenbosch University, Private Bag X1, Matieland, 7602, South Africa. ahitz@sun.ac.za
Abstract:Reactive oxygen species (ROS)-mediated damage has been hypothesized to play a role in the development and poor outcome of schizophrenia, as well as the development of neuroleptic-induced abnormal involuntary movements. Recently, the functional polymorphism (Ala-9Val) in the manganese superoxide dismutase (MnSOD) gene (part of the antioxidant defense mechanism) was found to be associated with schizophrenia in a Turkish population. This study was aimed at replicating this finding in a Xhosa population. In addition, the role of Ala-9Val in abnormal involuntary movement and tardive dyskinesia development in the Xhosa population was also investigated. The schizophrenic patient group (n=286) and a healthy control group (n=243) were genotyped for the Ala-9Val polymorphism using heteroduplex-single stranded conformational polymorphism (HEX-SSCP) analysis. No significant difference in genotype or allele frequency could be observed between the schizophrenia and control group (P=0.294 and P=0.528 respectively). In addition no association could be found between the polymorphism and symptom severity (SANS and SAPS). The Xhosa schizophrenia patient group with abnormal involuntary movements (n=54) and a subgroup with tardive dyskinesia (n=30) was found to significantly differ in Ala-9Val genotype frequency (P=0.008 and P=0.011 respectively) compared to the Xhosa schizophrenia patient group without abnormal involuntary movements (n=204). However, no significant difference was found for the allele frequencies (P=0.955 and P=0.161). Further, using ANCOVA no association was found between AIMS score and genotype in the group with abnormal involuntary movements (P=0.1234). However, in the patient group with tardive dyskinesia an association was observed between genotype and AIMS score (P=0.0365). These results do not support a major role of the MnSOD Ala-9Val polymorphism in the development of schizophrenia or symptom severity in the Xhosa population. Yet it seems to be involved in the development of abnormal involuntary movements and tardive dyskinesia and may even modulate the severity of tardive dyskinesia.
Keywords:·OH  hydroxyl radical  A  adenine  AIM  abnormal involuntary movements  AIM−  without abnormal involuntary movements  AIM+  with abnormal involuntary movements  AIMS  abnormal involuntary movement scale  Ala  alanine  ANCOVA  analysis of covariance  BHPR  Bunney–Hamburg Psychosis Rating  bp  basepairs  BPRS  Brief Psychiatric Rating Scale  C  cytosine  CAT  catalase  CNS  central nervous system  DIGS  Diagnostic Interview for Genetic Studies  DNA  deoxyribonucleic acid  dNTP  deoxynucleoside triphosphate  DRD3  dopamine D3 receptor  DSM-IV  Diagnostic and Statistical Manual of Mental Disorders  fourth edition  G  guanine  Gly  glycine  GSHPx  glutathione peroxidase  H2O2  hydrogen peroxide  HEX-SSCP  heteroduplex-single strand conformational polymorphism  HWE  Hardy–Weinberg equilibrium  MgCl2  magnesium chloride  MnSOD  manganese superoxide dismutase  MTS  mitochondrial targetting sequence  n  number  NH4  ammonium  O2  superoxide radical  PANSS  Positive and Negative Syndrome Scale  PCR  polymerase chain reaction  PUFAs  polyunsaturated fatty acids  ROS  reactive oxygen species  SANS  Scale for the Assessment of Negative Symptoms  SAPS  Scale for the Assessment of Positive Symptoms  Ser  serine  SOD  superoxide dismutase  SPSS  Statistical Package for the Social Sciences  T  thymine  TBARS  thiobarbituric acid reactive substances  TD  tardive dyskinesia  TD+  tardive dyskinesia positive  TFPGA  Tools for Population Genetic Analysis  UV  ultraviolet  Val  valine  
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