• Title of article

    Association of An Orexin 1 Receptor 408Val Variant with Polydipsia–Hyponatremia in Schizophrenic Subjects

  • Author/Authors

    Joanne Meerabux، نويسنده , , Yoshimi Iwayama-Shigeno، نويسنده , , Takeshi Sakurai، نويسنده , , Hisako Ohba، نويسنده , , Tomoko Toyota، نويسنده , , Kazuo Yamada، نويسنده , , Ruby Nagata، نويسنده , , Yoko Irukayama-Tomobe، نويسنده , , Hiromitsu Shimizu، نويسنده , , Kiyoshi Yoshitsugu، نويسنده , , Katsuya Ohta، نويسنده , , Takeo Yoshikawa، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2005
  • Pages
    7
  • From page
    401
  • To page
    407
  • Abstract
    Background Primary polydipsia is a common complication in patients with chronic psychoses, particularly schizophrenia. Disease pathogenesis is poorly understood, but one contributory factor is thought to be dopamine dysregulation caused by prolonged treatment with neuroleptics. Both angiotensin-converting enzyme (ACE) and orexin (hypocretin) signaling can modulate drinking behavior through interactions with the dopaminergic system. Methods We performed association studies on the insertion/deletion (I/D) sequence polymorphism of ACE and single nucleotide polymorphisms within the prepro-orexin (HCRT), orexin receptor 1 (HCRTR1), and orexin receptor 2 (HCRTR2) genes. Genotypes were determined by polymerase chain reaction amplification, followed by either electrophoretic separation or direct sequencing. Results The ACE I/D polymorphism showed no association with polydipsic schizophrenia. Screening of the orexin signaling system detected a 408 isoleucine to valine mutation in HCRTR1 that showed significant genotypic association with polydipsic–hyponatremic schizophrenia (p = .012). The accumulation of this mutation was most pronounced in polydipsic versus nonpolydipsic schizophrenia (p = .0002 and p = .008, for the respective genotypic and allelic associations). The calcium mobilization properties and the protein localization of mutant HCRTR1 seem to be unaltered. Conclusion Our preliminary data suggest that mutation carriers might have an increased susceptibility to polydipsia through an undetermined mechanism.
  • Keywords
    Schizophrenia , Drinking behavior , neuroleptics , hypocretin , angiotensin-converting enzyme , dopamine system
  • Journal title
    Biological Psychiatry
  • Serial Year
    2005
  • Journal title
    Biological Psychiatry
  • Record number

    502780